Your search keyword '"Tissue Distribution"' showing total 185,924 results

201. Pharmacokinetic profiles of 3- ( 4-hydroxy-3-methoxyphenyl ) propionic acid and its conjugates in Sprague-Dawley rats.

Author

Chizumi Abe, Ayano Soma, Tint Ni Ni Tun, Ye Zhang, Yosuke Nishitani, Hiroyuki Kayaki, Hideaki Kawakami, and Toshiro Matsui

Subjects

*PROPIONIC acid, *SPRAGUE Dawley rats, *PHARMACOKINETICS, *GUT microbiome, *TISSUE metabolism, *THORACIC aorta, *SOLEUS muscle

Abstract

3- ( 4-hydroxy-3-methoxyphenyl ) propionic acid ( HMPA ) is one of the end-products from gut microbiota from dietary polyphenols, which might contribute to their health benefits. This study aims to investigate the absorption, metabolism, and tissue accumulation of HMPA in Sprague-Dawley ( SD ) rats. After HMPA ( 10 mg/kg body weight ) was orally administered, intact and conjugated HMPAs in the bloodstream were detected and reached the maximum concentration in 15 min ( HMPA, 2.6 ± 0.4 nmol/mL; sulfated HMPA, 3.6 ± 0.9 nmol/mL; glucuronidated HMPA, 0.55 ± 0.09 nmol/mL ) . HMPA and its conjugates were also detected in the target organs 6 h postadministration, indicating that HMPA undergoes rapid conversion into conjugates, and they broadly distribute to organs with similar profiles ( kidneys > liver > thoracic aorta > heart > soleus muscle > lungs ) . This study demonstrated that orally administered HMPA ( 10 mg/kg ) in SD rats undergoes rapid metabolism and wide tissue distribution with ≥1.2% absorption ratio. [ABSTRACT FROM AUTHOR]

Published

2023

202. Dynamic Distribution of Mesanophrys sp. and Tissue Enzyme Activities in Experimentally Infected Mud Crab Scylla paramamosain.

Author

Zhang, Kexin, Zhang, Weiren, Li, Ronghua, Lu, Junkai, Chen, Qingwei, Hu, Haojie, Yin, Fei, Mu, Changkao, Song, Weiwei, and Wang, Chunlin

Subjects

*SCYLLA (Crustacea), *SURVIVAL rate, *NERVE tissue, *POLYMERASE chain reaction, *CATALASE, *SUPEROXIDE dismutase

Abstract

Mesanophrys sp. is reported to be highly pathogenic to marine crustaceans. This study presents the first report of Mesanophrys sp. infection in the mud crab (Scylla paramamosain). In this study, we first recorded the survival rates of an experimentally infected group and a control group; the cumulative survival rate in the infected group was significantly lower compared to the control group after 72 h (73.20% vs. 94.19%), while the highest mortality of S. paramamosain occurred within the first 24 h post-infection. Then, we investigated the dynamic distribution and tissue tropism of the Mesanophrys sp. in the infected S. paramamosain by a quantitative real-time polymerase chain reaction (qPCR). The result showed that a significant increase in the number of Mesanophrys sp. could be detected in all tested tissues (obtained from the eyestalks, gills, heart, nerves, muscles and hepatopancreas) at 3 h post-infection. The numbers of Mesanophrys sp. in the gill, eyestalk and nerve tissues were relatively higher than in the other tissues. The gill tissue showed the highest numbers from 6 to 48 h. Histopathological observation found a severe collapse in the filament structure, which indicated tissue-specific pathogen infection. Furthermore, the antioxidant enzyme activity of superoxide dismutase (SOD), catalase (CAT) and peroxidase (POD) in three representative tissues (gill, muscle and hepatopancreas) were compared between the infected and control groups, and a significant increase in enzyme activity was observed in all three tested tissues in the infected group, indicating a relatively strong innate immune defense reaction that could have been induced by Mesanophrys sp. infection. These results will be helpful to Mesanophrys sp. pathogenicity-related research and the control of this pathogen in S. Paramamosain in the future. [ABSTRACT FROM AUTHOR]

Published

2023

203. The tissue distribution of Jinzhen oral liquid in healthy and influenza mice.

Author

Chen, Xialin, Gao, Xia, Cao, Liang, Wang, Shanli, Qian, Mengyu, Tong, Xiaoyu, Wang, Jiajia, Gao, Huifang, Wang, Zhenzhong, Li, Jifeng, and Xiao, Wei

Abstract

Jinzhen oral liquid (JZOL) is widely used in China. However, its tissue distribution, a vital part of the efficacy substances research, has not been reported yet. This study characterized its chemical components and its prototypes and metabolites in mice, and investigated its tissue distribution in pathological and healthy mice. Several constituents were characterized, including 55 constituents in JZOL, 11 absorbed prototypes and six metabolites in plasma and tissues. The metabolic pathways were demethylation, dehydration and acetylation. A sensitive, accurate and stable quantitative method was established and applied to the tissue distribution. After administration of JZOL, these seven components were rapidly distributed to various tissues, mainly staying in the small intestine, and less distributed to lung, liver and kidney. Compared with healthy mice, the absorption of baicalin, wogonoside, rhein, glycyrrhizic acid and liquiritin apioside was reduced in influenza mice, but their elimination was slow. However, influenza infection had no obvious effect on the overall distribution of the most important components (baicalin, glycyrrhizic acid and wogonoside) in the plasma or small intestine, but obviously affected the distribution of baicalin in liver. In summary, seven components are rapidly distributed to various tissues, and influenza infection has certain influence on the tissue distribution of JZOL. [ABSTRACT FROM AUTHOR]

Published

2023

204. Distribution of Micro-Nano PS, DEHP, and/or MEHP in Mice and Nerve Cell Models In Vitro after Exposure to Micro-Nano PS and DEHP.

Author

Han, Jie, Yan, Jun, Li, Kang, Lin, Bencheng, Lai, Wenqing, Bian, Liping, Jia, Rui, Liu, Xiaohua, and Xi, Zhuge

Subjects

NEURONS, MICE, PARTICLE size distribution

Abstract

Polystyrene (PS) and di-(2-ethylhexyl) phthalate (DEHP) exist widely in the environment. However, their distribution in organisms remains unclear. We used three sizes (50 nm, 500 nm, and 5 μm) of PS and DEHP to study the distribution and accumulation of PS, DEHP, and mono(2-ethylhexyl) phthalate (MEHP) in mice and nerve cell models (HT22 and BV2 cells) and their potential toxicity. Results showed that PS entered the blood of mice, and the distribution of different particle sizes in different tissues was different. After the combined exposure to PS and DEHP, PS carried DEHP, which significantly increased the DEHP content and MEHP content and the highest content of MEHP was in the brain. With the decrease in PS particle size, the contents of PS, DEHP, and MEHP in the body increased. The levels of inflammatory factors were increased in the serum of the PS or/and DEHP group. In addition, 50 nm polystyrene can carry MEHP into nerve cells. These results suggest for the first time that PS and DEHP combined exposure can induce systemic inflammation, and the brain is an important target organ of PS and DEHP combined exposure. This study may serve as a reference for further evaluation of the neurotoxicity induced by combined exposure to PS and DEHP. [ABSTRACT FROM AUTHOR]

Published

2023

205. Physiologically Based Pharmacokinetic Modeling to Characterize the Effect of Molecular Charge on Whole-Body Disposition of Monoclonal Antibodies.

Author

Liu, Shufang and Shah, Dhaval K.

Abstract

Motivated by a series of work demonstrating the effect of molecular charge on antibody pharmacokinetics (PK), physiological-based pharmacokinetic (PBPK) models are emerging that relate in silico calculated charge or in vitro measures of polyspecificity to antibody PK parameters. However, only plasma data has been used for model development in these studies, leading to unvalidated assumptions. Here, we present an extended platform PBPK model for antibodies that incorporate charge-dependent endothelial cell pinocytosis rate and nonspecific off-target binding in the interstitial space and on circulating blood cells, to simultaneously characterize whole-body disposition of three antibody charge variants. Predictive potential of various charge metrics was also explored, and the difference between positive charge patches and negative charge patches (i.e., PPC-PNC) was used as the charge parameter to establish quantitative relationships with nonspecific binding affinities and endothelial cell uptake rate. Whole-body disposition of these charge variants was captured well by the model, with less than 2-fold predictive error in area under the curve of most plasma and tissue PK data. The model also predicted that with greater positive charge, nonspecific binding was more substantial, and pinocytosis rate increased especially in brain, heart, kidney, liver, lung, and spleen, but remained unchanged in adipose, bone, muscle, and skin. The presented PBPK model contributes to our understanding of the mechanisms governing the disposition of charged antibodies and can be used as a platform to guide charge engineering based on desired plasma and tissue exposures. [ABSTRACT FROM AUTHOR]

Published

2023

206. Benzisothiazolinone: Pharmacokinetics, Tissue Distribution, and Mass Balance Studies in Rats.

Author

Jo, Seong Jun, Bae, Soo Hyeon, Huang, Zhouchi, Lee, Sangyoung, Lee, Chae Bin, Chae, Soon Uk, Park, Jung Bae, Kwon, Mihye, Chung, Hye Kyung, and Bae, Soo Kyung

Subjects

PHARMACOKINETICS, SKIN absorption, RATS, DIGESTIVE organs, TISSUES, LUNGS

Abstract

Humans are continuously exposed to benzisothiazolinone (BIT), which is used as a preservative, through multiple routes. BIT is known to be a sensitizer; in particular, dermal contact or aerosol inhalation could affect the local toxicity. In this study, we evaluated the pharmacokinetic properties of BIT in rats following various routes of administration. BIT levels were determined in rat plasma and tissues after oral inhalation and dermal application. Although the digestive system rapidly and completely absorbed orally administered BIT, it underwent severe first-pass effects that prevented high exposure. In an oral dose escalation study (5–50 mg/kg), nonlinear pharmacokinetic properties showed that Cmax and the area under the curve (AUC) increased more than dose proportionality. In the inhalation study, the lungs of rats exposed to BIT aerosols had higher BIT concentrations than the plasma. Additionally, the pharmacokinetic profile of BIT after the dermal application was different; continuous skin absorption without the first-pass effect led to a 2.13-fold increase in bioavailability compared with oral exposure to BIT. The [14C]-BIT mass balance study revealed that BIT was extensively metabolized and excreted in the urine. These results can be used in risk assessments to investigate the relationship between BIT exposure and hazardous potential. [ABSTRACT FROM AUTHOR]

Published

2023

207. Use of physiological based pharmacokinetic modeling for cross-species prediction of pharmacokinetic and tissue distribution profiles of a novel niclosamide prodrug.

Author

Mengbi Yang, Wang, Amy Q., Padilha, Elias C., Shah, Pranav, Hagen, Natalie R., China Ryu, Shamim, Khalida, Wenwei Huang, and Xin Xu

Subjects

PHARMACOKINETICS, ORAL drug administration, LUNGS, DRUG repositioning, INTRAVENOUS therapy, ANTHELMINTICS

Abstract

Introduction: Niclosamide (Nc) is an FDA-approved anthelmintic drug that was recently identified in a drug repurposing screening to possess antiviral activity against SARS-CoV-2. However, due to the low solubility and permeability of Nc, its in vivo efficacy was limited by its poor oral absorption. Method: The current study evaluated a novel prodrug of Nc (PDN; NCATSSM4705) in improving in vivo exposure of Nc and predicted pharmacokinetic profiles of PDN and Nc across different species. ADME properties of the prodrug were determined in humans, hamsters, and mice, while the pharmacokinetics (PK) of PDN were obtained in mice and hamsters. Concentrations of PDN and Nc in plasma and tissue homogenates were measured by UPLC-MS/MS. A physiologically based pharmacokinetic (PBPK) model was developed based on physicochemical properties, pharmacokinetic and tissue distribution data in mice, validated by the PK profiles in hamsters and applied to predict pharmacokinetic profiles in humans. Results: Following intravenous and oral administration of PDN in mice, the total plasma clearance (CLp) and volume of distribution at steady-state (Vdss) were 0.061-0.063 L/h and 0.28-0.31 L, respectively. PDN was converted to Nc in both liver and blood, improving the systemic exposure of Nc in mice and hamsters after oral administration. The PBPK model developed for PDN and in vivo formed Nc could adequately simulate plasma and tissue concentration-time profiles in mice and plasma profiles in hamsters. The predicted human CLp/F and Vdss/F after an oral dose were 2.1 L/h/kg and 15 L/kg for the prodrug respectively. The predicted Nc concentrations in human plasma and lung suggest that a TID dose of 300 mg PDN would provide Nc lung concentrations at 8- to 60-fold higher than in vitro IC50 against SARS-CoV-2 reported in cell assays. Conclusion: In conclusion, the novel prodrug PDN can be efficiently converted to Nc in vivo and improves the systemic exposure of Nc in mice after oral administration. The developed PBPK model adequately depicts the mouse and hamster pharmacokinetic and tissue distribution profiles and highlights its potential application in the prediction of human pharmacokinetic profiles. [ABSTRACT FROM AUTHOR]

Published

2023

208. Differences in tissue distribution ability of evodiamine and dehydroevodiamine are due to the dihedral angle of the molecule stereo-structure.

Author

Jie Luo, Wen Wen, Jie Chen, Xiaobo Zeng, Ping Wang, and Shijun Xu

Subjects

DIHEDRAL angles, ELECTRIC potential, INTRAVENOUS injections, TISSUES, SKIN permeability, BLOOD-brain barrier, MOLECULES

Abstract

Introduction: This researcher focused at the evodiamine and dehydroevodiamine tissue distribution and structure-pharmacokinetics (PK) relationship after intravenous injection in mice. Methods: Using a transmembrane transport experiment, the permeability of evodiamine and dehydroevodiamine on Caco-2 cells was evaluated. The tissue distribution and pharmacokinetics (PK) of evodiamine and dehydroevodiamine in mice were studied. To comprehend the connection between structure and tissue distribution, physicochemical property evaluations and molecular electrostatic potential (MEP) calculations were performed. Results: Dehydroevodiamine's Papp values in vitro were 10-5 cm/s, whereas evodiamine's were 10-6 cm/s. At a dose of 5 mg/kg, the brain concentration of dehydroevodiamine was 6.44 times more than that of evodiamine. By MEP or physicochemical measures, the permeability difference between evodiamine and dehydroevodiamine is unaffected. The dihedral angle of the stereo-structure appears to be the main cause of the difference in tissue distribution ability between evodiamine and dehydroevodiamine. Discussion: Dehydroevodiamine has a dihedral angle of 3.71° compared to 82.34° for evodiamine. Dehydroevodiamine can more easily pass through the phospholipid bilayer than evodiamine because it has a more planar stereo-structure. Dehydroevodiamine is therefore more likely to pass cross the blood-brain barrier and enter the brain in a tissue-specific manner. [ABSTRACT FROM AUTHOR]

Published

2023

209. Regional distributions of curcumin and tetrahydrocurcumin in the liver and small intestine of rats when orally co‐administered with quercetin and paeoniflorin.

Author

Yu, Weilan, Liu, Xiaolin, Cai, Dake, Zheng, Juntao, Lao, Biaochang, Huang, Min, and Zhong, Guoping

Subjects

*SMALL intestine, *LIQUID chromatography-mass spectrometry, *CURCUMIN, *QUERCETIN

Abstract

Curcumin (CUR), derived from the dietary spice turmeric, is a polyphenolic compound with various biological and pharmacological activities. Tetrahydrocurcumin (THC) is one of the major reductive metabolites of curcumin. A pharmacokinetic study using ultra‐high‐performance liquid chromatography‐tandem mass spectrometry (UHPLC‐MS/MS) for the simultaneous determination of curcumin, THC, quercetin (QR), and paeoniflorin (PF) in rat plasma had been performed. In this study, the regional distributions of curcumin and tetrahydrocurcumin in the liver and the three segments of small intestine (duodenum, jejunum, and ileum) of rats when orally co‐administered with quercetin and paeoniflorin were carried out. Drug concentrations were determined using UHPLC‐MS/MS. The results showed that curcumin was well distributed in the small intestine, while the distributions of tetrahydrocurcumin in the liver, duodenum, jejunum were similar, but much more abundant in the ileum. When orally co‐administered with quercetin and paeoniflorin, the tissue to plasma concentration ratios (Kp values) of curcumin in the three segments of the small intestine were increased, indicating that the presence of quercetin and paeoniflorin increases the distribution of curcumin in these regions. Moreover, the half‐life (t1/2) of THC in the liver was significantly prolonged, and the Kp value of THC in the liver was increased and the Kp values in the small intestine were decreased, suggesting that the combination of quercetin and paeoniflorin might suppress the metabolism of curcumin in the small intestine. In brief, the combination had an effect on the distributions of curcumin and tetrahydrocurcumin in the liver and small intestine of rats. [ABSTRACT FROM AUTHOR]

Published

2023

210. 鸡 NLRC3 分子结构及其在宿主感染后的转录特征研究.

Author

张佳琪, 铁子月, 缪鑫雨, 张小荣, 吴艳涛, and 郭梦娇

Subjects

IMMUNOREGULATION, CHICKENS, TERTIARY structure, GENE expression, BACTERIAL diseases

Abstract

Copyright of Chinese Journal of Preventive Veterinary Medicine / Zhongguo Yufang Shouyi Xuebao is the property of Chinese Journal of Preventive Veterinary Medicine Editorial Office and its content may not be copied or emailed to multiple sites or posted to a listserv without the copyright holder's express written permission. However, users may print, download, or email articles for individual use. This abstract may be abridged. No warranty is given about the accuracy of the copy. Users should refer to the original published version of the material for the full abstract. (Copyright applies to all Abstracts.)

Published

2023

211. Biokinetics of subacutely co-inhaled same size gold and silver nanoparticles.

Author

Lee, Philku, Kim, Jin Kwon, Jo, Mi Seong, Kim, Hoi Pin, Ahn, Kangho, Park, Jung Duck, Gulumian, Mary, Oberdörster, Günter, and Yu, Il Je

Subjects

GOLD nanoparticles, SILVER nanoparticles, OLFACTORY cortex, NANOPARTICLE size, SPRAGUE Dawley rats, ORGANS (Anatomy), OLFACTORY bulb

Abstract

Background: Toxicokinetics of nanomaterials, including studies on the absorption, distribution, metabolism, and elimination of nanomaterials, are essential in assessing their potential health effects. The fate of nanomaterials after inhalation exposure to multiple nanomaterials is not clearly understood. Methods: Male Sprague–Dawley rats were exposed to similar sizes of silver nanoparticles (AgNPs, 10.86 nm) and gold nanoparticles (AuNPs, 10.82 nm) for 28 days (6-h/day, 5-days/week for four weeks) either with separate NP inhalation exposures or with combined co-exposure in a nose-only inhalation system. Mass concentrations sampled from the breathing zone were AuNP 19.34 ± 2.55 μg/m3 and AgNP 17.38 ± 1.88 μg/m3 for separate exposure and AuNP 8.20 μg/m3 and AgNP 8.99 μg/m3 for co-exposure. Lung retention and clearance were previously determined on day 1 (6-h) of exposure (E-1) and on post-exposure days 1, 7, and 28 (PEO-1, PEO-7, and PEO-28, respectively). In addition, the fate of nanoparticles, including translocation and elimination from the lung to the major organs, were determined during the post-exposure observation period. Results: AuNP was translocated to the extrapulmonary organs, including the liver, kidney, spleen, testis, epididymis, olfactory bulb, hilar and brachial lymph nodes, and brain after subacute inhalation and showed biopersistence regardless of AuNP single exposure or AuNP + AgNP co-exposure, showing similar elimination half-time. In contrast, Ag was translocated to the tissues and rapidly eliminated from the tissues regardless of AuNP co-exposure. Ag was continually accumulated in the olfactory bulb and brain and persistent until PEO-28. Conclusion: Our co-exposure study of AuNP and AgNP indicated that soluble AgNP and insoluble AuNP translocated differently, showing soluble AgNP could be dissolved into Ag ion to translocate to the extrapulmonary organs and rapidly removed from most organs except the brain and olfactory bulb. Insoluble AuNPs were continually translocated to the extrapulmonary organs, and they were not eliminated rapidly. [ABSTRACT FROM AUTHOR]

Published

2023

212. Danggui Buxue Decoction: Comparative pharmacokinetic research on six bio‐active components in different states by ultra‐performance liquid chromatography‐tandem mass spectrometry after oral administration.

Author

Zhao, Hedi, Qi, Miao, Gong, Yuan, Chen, Han, Wang, Dan, Fan, Jing, Wang, Yanmin, and Wang, Jingjuan

Subjects

*ORAL drug administration, *LIQUID chromatography-mass spectrometry, *PHARMACOKINETICS, *MOLECULAR weights, *BLOOD proteins, *PROTEIN binding, *CHINESE medicine

Abstract

Danggui Buxue Decoction is a classic formula containing Astragali Radix and Angelicae Sinensis Radix in a 5:1 ratio and has been extensively used to treat blood deficiency for thousands of years. The aim of the study was to investigate the differences in plasma protein binding, pharmacokinetics, and tissue distribution of Danggui Buxue Decoction in normal and blood‐deficient rats by ultra‐performance liquid chromatography‐tandem mass spectrometry. The effects on peripheral blood routine were verified. The compounds exhibited higher plasma protein binding and absorption in the model group compared to the control group, except formononetin. The six ingredients were distributed widely, and the highest concentrations were detected in the heart and uterus. As has been demonstrated in the previous study of the effect of Danggui Buxue Decoction, its potential is to serve as an effective traditional Chinese medicine formula for treating cardiovascular diseases and impacting estrogenic properties, which reveals the potential target organs of Danggui Buxue Decoction the heart and uterus. Our findings suggested that the absorption and distribution of different components in Danggui Buxue Decoction varies depending on the pathological state, molecular weight, lipid solubility, transporter‐mediated efflux, and other factors. [ABSTRACT FROM AUTHOR]

Published

2023

213. Change of metformin concentrations in the liver as a pharmacological target site of metformin after long-term combined treatment with ginseng berry extract.

Author

Choong Whan Lee, Byoung Hoon You, Sreymom Yim, Seung Yon Han, Hee-Sung Chae, Mingoo Bae, Seo-Yeon Kim, Jeong-Eun Yu, Jieun Jung, Piseth Nhoek, Hojun Kim, Han Seok Choi, Young-Won Chin, Hyun Woo Kim, and Young Hee Choi

Subjects

BERRIES, METFORMIN, GINSENG, DRUG interactions, LIVER, ORAL medication, ENTEROHEPATIC circulation

Abstract

Metformin as an oral glucose-lowering drug is used to treat type 2 diabetic mellitus. Considering the relatively high incidence of cardiovascular complications and other metabolic diseases in diabetic mellitus patients, a combination of metformin plus herbal supplements is a preferrable way to improve the therapeutic outcomes of metformin. Ginseng berry, the fruit of Panax ginseng Meyer, has investigated as a candidate in metformin combination mainly due to its anti-hyperglycemic, anti-hyperlipidemic, antiobesity, anti-hepatic steatosis and anti-inflammatory effects. Moreover, the pharmacokinetic interaction of metformin via OCTs and MATEs leads to changes in the efficacy and/or toxicity of metformin. Thus, we assessed how ginseng berry extract (GB) affects metformin pharmacokinetics in mice, specially focusing on the effect of the treatment period (i.e., 1-day and 28-day) of GB on metformin pharmacokinetics. In 1-day and 28-day co-treatment of metformin and GB, GB did not affect renal excretion as a main elimination route of metformin and GB therefore did not change the systemic exposure of metformin. Interestingly, 28-day co-treatment of GB increased metformin concentration in the livers (i.e., 37.3, 59.3% and 60.9% increases versus 1-day metformin, 1-day metformin plus GB and 28-day metformin groups, respectively). This was probably due to the increased metformin uptake via OCT1 and decreased metformin biliary excretion via MATE1 in the livers. These results suggest that co-treatment of GB for 28 days (i.e., long-term combined treatment of GB) enhanced metformin concentration in the liver as a pharmacological target tissue of metformin. However, GB showed a negligible impact on the systemic exposure of metformin in relation to its toxicity (i.e., renal and plasma concentrations of metformin). [ABSTRACT FROM AUTHOR]

Published

2023

214. Pharmacokinetics and tissue distribution of bleomycin-induced idiopathic pulmonary fibrosis rats treated with cryptotanshinone.

Author

Xiangjun He, Zhi Zhong, Quan Wang, Zhenmao Jia, Jing Lu, Jianwen Chen, and Peiqing Liu

Subjects

IDIOPATHIC pulmonary fibrosis, LUNGS, ORAL drug administration, PULMONARY fibrosis, RATS, SALVIA miltiorrhiza, LIQUID chromatography-mass spectrometry, PHARMACOKINETICS

Abstract

Introduction: Cryptotanshinone(CTS), a compound derived from the root of Salvia miltiorrhiza, has been linked to various of diseases, particularly pulmonary fibrosis. In the current study, we investigated the benefit of CTS on Sprague-Dawley (SD) rats induced by bleomycin (BLM) and established high performance liquid chromatography-tandem mass spectrometry (HPLC-MS/ MS) methods to compare pharmacokinetics and tissue distribution in subsequent normal and modulated SD rats. Methods: The therapeutic effect of CTS on BLM-induced SD rats was evaluated using histopathology, lung function and hydroxyproline content measurement, revealing that CTS significantly improved SD rats induced by BLM. Additionally, a simple, rapid, sensitive and specific HPLC-MS/MS method was developed to determine the pharmacokinetics of various components in rat plasma. Results: Pharmacokinetic studies indicated that CTS was slowly absorbed by oral administration and had low bioavailability and a slow clearance rate. The elimination of pulmonary fibrosis in 28-day rats was slowed down, and the area under the curve was increased compared to the control group. Longterm oral administration of CTS did not accumulate in vivo, but the clearance was slowed down, and the steady-state blood concentration was increased. The tissue distribution study revealed that CTS exposure in the lungs and liver. Discussion: The lung CTS exposure was significantly higher in the model group than in the control group, suggesting that the pathological changes of pulmonary fibrosis were conducive to the lung exposure of CTS and served as the target organ of CTS. [ABSTRACT FROM AUTHOR]

Published

2023

215. Tumour, whole‐blood, plasma and tissue concentrations of metformin in lung cancer patients.

Author

Phillips, Joseph D., Pooler, Darcy B., Ness, Dylan B., Fay, Kayla, Tau, Steven, Demidenko, Eugene, Hampsch, Riley A., Lewis, Lionel D., and Miller, Todd W.

Subjects

*LIQUID chromatography-mass spectrometry, *METFORMIN, *LUNGS, *LUNG cancer, *TYPE 2 diabetes

Abstract

Aim: Metformin is used for the management of type 2 diabetes mellitus (T2DM) and is being tested clinically as an anticancer agent. Metformin concentrations safely achievable in human solid tissues including tumours are unknown. This study was designed to determine metformin concentration in tissue compartments as a function of dose to inform rational dosing in preclinical models and interpretation of clinical results." Methods: Subjects with solid tumours to be treated by resection and either (A) willingness to take metformin for 7‐10 days before surgery or (B) taking metformin for T2DM were eligible. Whole blood, plasma, tumour, tumour‐adjacent uninvolved tissue and subcutaneous adipose tissue were obtained for liquid chromatography with tandem mass spectrometry to measure metformin concentrations. Results: All subjects had primary lung tumours. Metformin dose was significantly correlated with drug concentrations in all tissues analysed. Intersubject metformin concentrations varied by over two orders of magnitude. Metformin concentrations were significantly higher in tumour tissues and lower in adipose tissues compared to other tissues. Concentrations in blood and plasma were significantly correlated with concentrations in solid tissues. Conclusion: Metformin accumulates in cellular compartments. Concentrations observed in plasma, blood, lung and tumour tissues in subjects treated with US Food and Drug Administration‐approved doses for T2DM are lower than those typically used in tissue culture studies. However, such tissue concentrations are in line with those found within cultured cells treated with supra‐pharmacological doses of metformin. Given the large intersubject variability in metformin concentrations, it is imperative to determine whether there is an association between tissue metformin concentration and anticancer activity in humans. [ABSTRACT FROM AUTHOR]

Published

2023

216. Study on Absorption, Distribution and Excretion of a New Candidate Compound XYY-CP1106 against Alzheimer's Disease in Rats by LC-MS/MS.

Author

Guo, Zili, Gao, Bianbian, Fan, Miaoliang, Chen, Lisha, Zhang, Changjun, Liang, Xianrui, Su, Weike, and Xie, Yuanyuan

Subjects

*ALZHEIMER'S disease, *NEUROFIBRILLARY tangles, *RAT diseases, *LIQUID chromatography-mass spectrometry, *EXCRETION, *ORAL drug administration

Abstract

XYY-CP1106, a candidate compound synthesized from a hybrid of hydroxypyridinone and coumarin, has been shown to be remarkably effective in treating Alzheimer's disease. A simple, rapid and accurate high-performance liquid chromatography coupled with the triple quadrupole mass spectrometer (LC-MS/MS) method was established in this study to elucidate the pharmacokinetics of XYY-CP1106 after oral and intravenous administration in rats. XYY-CP1106 was shown to be rapidly absorbed into the blood (Tmax, 0.57–0.93 h) and then eliminated slowly (T1/2, 8.26–10.06 h). Oral bioavailability of XYY-CP1106 was (10.70 ± 1.72)%. XYY-CP1106 could pass through the blood–brain barrier with a high content of (500.52 ± 260.12) ng/g at 2 h in brain tissue. The excretion results showed that XYY-CP1106 was mainly excreted through feces, with an average total excretion rate of (31.14 ± 0.05)% in 72 h. In conclusion, the absorption, distribution and excretion of XYY-CP1106 in rats provided a theoretical basis for subsequent preclinical studies. [ABSTRACT FROM AUTHOR]

Published

2023

217. ABCG2 transporter plays a key role in the biodistribution of melatonin and its main metabolites.

Author

Álvarez‐Fernández, Laura, Gomez‐Gomez, Alex, Haro, Noemí, García‐Lino, Alba M., Álvarez, Ana I., Pozo, Oscar J., and Merino, Gracia

Subjects

*ATP-binding cassette transporters, *ORAL drug administration, *METABOLITES, *MELATONIN, *LACTATION, *XENOBIOTICS

Abstract

The ATP‐binding cassette G2 (ABCG2) is an efflux transporter expressed in the apical membrane of cells from a large number of tissues, directly affecting bioavailability, tissue accumulation, and secretion into milk of both xenobiotics and endogenous compounds. The aim of this work was to characterize the role of ABCG2 in the systemic distribution and secretion into milk of melatonin and its main metabolites, 6‐hydroxymelatonin, and 6‐sulfatoxymelatonin. For this purpose, we first showed that these three molecules are transported by this transporter using in vitro transepithelial assays with MDCK‐II polarized cells transduced with different species variants of ABCG2. Second, we tested the in vivo effect of murine Abcg2 in the systemic distribution of melatonin and its metabolites using wild‐type and Abcg2−/− mice. Our results show that after oral administration of melatonin, the plasma concentration of melatonin metabolites in Abcg2−/− mice was between 1.5 and 6‐fold higher compared to the wild‐type mice. We also evaluated in these animals differences in tissue accumulation of melatonin metabolites. The most relevant differences between both types of mice were found for small intestine and kidney (>sixfold increase for 6‐sulfatoxymelatonin in Abcg2−/− mice). Finally, melatonin secretion into milk was also affected by the murine Abcg2 transporter, with a twofold higher milk concentration in wild‐type compared with Abcg2−/− lactating female mice. In addition, melatonin metabolites showed a higher milk‐to‐plasma ratio in wild‐type mice. Overall, our results show that the ABCG2 transporter plays a critical role in the biodistribution of melatonin and its main metabolites, thereby potentially affecting their biological and therapeutic activity. [ABSTRACT FROM AUTHOR]

Published

2023

218. Genome-wide identification, phylogeny and expression analysis of the bmp gene family associated with development and skeleton deformity in cobia (Rachycentron canadum)

Author

Qian Ma, Yunsheng Yang, Feifan Mao, Qiling Zhou, Liuyong Wang, and Gang Chen

Subjects

BMP, Rachycentron canadum, Tissue distribution, Early developmental stages, Skeleton deformity, Aquaculture. Fisheries. Angling, SH1-691

Abstract

Bone morphogenetic proteins (BMPs) are critical for controlling skeletal development of fish, which has significant influence on external morphology, functional exercise and even survival rate in aquaculture breeding. In this study, a total of 19 bmp genes were identified in cobia (Rachycentron canadum) and these genes were divided into six sub-families according to phylogenetic analysis, including bmp1, bmp3/11/15, bmp2/4/16, bmp9/10, bmp13/14 and bmp5/6/7/8 subfamily. The identified cobia BMPs, excepting for BMP1, all possessed a similar TGF_beta domain. Phylogenetic analysis revealed that the cobia bmp genes were most closely related to those of the golden pompano (Trachinotus ovatus). The tissue distribution of these bmps in adult cobia revealed that the highest expression of most bmp genes was found in the Meckel’s cartilage; the highest expression of bmp4 was identified in the vertebrae; five other bmps were highly expressed in non-skeleton tissues including liver, heart and gill. The expression of bmp genes were also identified during the larvae and juvenile stages (1–30 dph), and most bmps revealed no certain expression pattern excepting for bmp8a, which showed significantly lower mRNA level before 15 dph and then increased to a significantly higher level. Due to the high incidence of deformity during the larvae and juvenile stages of cobia, the difference of bmp mRNA levels between deformed and normal skeletons (the Meckel’s cartilage and vertebrae) were also investigated to understand the involvement of bmp genes in skeletal deformity. The results showed that most of the bmp genes were significantly inhibited in the deformed Meckel’s cartilage excepting for bmp1, bmp5 and bmp7b; while in the deformed vertebrae, expression of most bmps were significantly increased excepting for five genes (bmp1, bmp4, bmp5, bmp7b and bmp13b).

Published

2023

219. Study on the Anti-Ulcerative Colitis Effect of Pseudo-Ginsenoside RT4 Based on Gut Microbiota, Pharmacokinetics, and Tissue Distribution

Author

Hui Yu, Caixia Wang, Junzhe Wu, Qianyun Wang, Hanlin Liu, Zhuoqiao Li, Shanmei He, Cuizhu Wang, and Jinping Liu

Subjects

RT4, ulcerative colitis, intestinal flora, pharmacokinetics, tissue distribution, Biology (General), QH301-705.5, Chemistry, QD1-999

Abstract

The purpose of this study was to explore the therapeutic effect of the oral administration of pseudo-ginsenoside RT4 (RT4) on ulcerative colitis (UC), and to determine the rate of absorption and distribution of RT4 in mice with UC. Balb/c mice were induced using dextran sulfate sodium salts (DSS) to establish the UC model, and 10, 20, or 40 mg/kg of RT4 was subsequently administered via gavage. The clinical symptoms, inflammatory response, intestinal barrier, content of total short-chain fatty acids (SCFAs), and gut microbiota were investigated. Caco-2 cells were induced to establish the epithelial barrier damage model using LPS, and an intervention was performed using 4, 8, and 16 µg/mL of RT4. The inflammatory factors, transient electrical resistance (TEER), and tight-junction protein expression were determined. Finally, pharmacokinetic and tissue distribution studies following the intragastric administration of RT4 in UC mice were performed. According to the results in mice, RT4 decreased the disease activity index (DAI) score, restored the colon length, reduced the levels of pro-inflammatory cytokines (TNF-α, IL-6, and IL-1β), and boosted the levels of immunosuppressive cytokine IL-10, increased the content of SCFAs, improved the colonic histopathology, maintained the ultrastructure of colonic mucosal epithelial cells, and corrected disturbances in the intestinal microbiota. Based on the results in caco-2 cells, RT4 reduced the levels of TNF-α, IL-6, and IL-1β; protected integrity of monolayers; and increased tight-junction protein expression. Additionally, the main pharmacokinetic parameters (Cmax, Tmax, t1/2, Vd, CL, AUC) were obtained, the absolute bioavailability was calculated as 18.90% ± 2.70%, and the main distribution tissues were the small intestine and colon. In conclusion, RT4, with the features of slow elimination and directional distribution, could alleviate UC by inhibiting inflammatory factors, repairing the intestinal mucosal barrier, boosting the dominant intestinal microflora, and modulating the expression of SCFAs.

Published

2024

220. Pharmacokinetic, Tissue Distribution, Metabolite, and Toxicity Evaluation of the Matrine Derivative, (6aS, 10S, 11aR, 11bR, 11cS)-10-Methylaminododecahydro-3a, 7a-Diaza-benzo (de) Anthracene-8-thione

Author

Liuyan Li, Fangfang Lu, Shuqin Ding, Xiaoying Wang, Weibiao Wang, Wannian Zhang, Weiheng Xu, Chunlin Zhuang, Zhenyuan Miao, and Xueqin Ma

Subjects

MASM, pharmacokinetics, tissue distribution, metabolites, toxicity evaluation, Organic chemistry, QD241-441

Abstract

MASM, a structurally modified derivative of matrine, exhibits superior efficacy in reducing inflammation and liver injury in rats when compared to matrine. This study aims to investigate the pharmacokinetic profile and acute toxicity of MASM. Pharmacokinetic results revealed that MASM exhibited rapid absorption, with a Tmax ranging from 0.21 ± 0.04 h to 1.31 ± 0.53 h, and was eliminated slowly, with a t1/2 of approximately 10 h regardless of the route of administration (intravenous, intraperitoneal, or intragastric). The absolute intragastric bioavailability of MASM in rats was determined to be 44.50%, which was significantly higher than that of matrine (18.5%). MASM was detected in all rat tissues including the brain, and through the utilization of stable isotope-labeled compounds and standard references, ten metabolites of MASM, namely sophocarpine, oxysophocarpine, and oxymatrine, were tentatively identified. The LD50 of MASM in mice was determined to be 94.25 mg/kg, surpassing that of matrine (83.21 mg/kg) based on acute toxicity results. Histopathological and biochemical analysis indicated no significant alterations in the primary organs of the low- to medium-dosage groups of MASM. These findings provide valuable insights into the efficacy and toxicity profile of MASM.

Published

2024

221. Absorption, Distribution, Metabolism, and Excretion of [14C]BS1801, a Selenium-Containing Drug Candidate, in Rats

Author

Cheng Yang, Mingzhen Xue, Yifei He, Hanwei Yin, Chen Yang, Dafang Zhong, Huihui Zeng, Yuandong Zheng, and Xingxing Diao

Subjects

[14C]BS1801, BS1801 (butaselen), tissue distribution, metabolism, mass balance, selenium, Organic chemistry, QD241-441

Abstract

BS1801 is a selenium-containing drug candidate with potential for treating liver and lung fibrosis. To fully elucidate the biotransformation of BS1801 in animals and provide sufficient preclinical drug metabolism data for human mass balance study, the metabolism of BS1801 in rats was investigated. We used radiolabeling techniques to investigate the mass balance, tissue distribution, and metabolite identification of BS1801 in Sprague–Dawley/Long–Evans rats after a single oral dose of 100 mg/kg (100 μCi/kg) [14C]BS1801: 1. The mean recovery of radioactive substances in urine and feces was 93.39% within 168 h postdose, and feces were the main excretion route. 2. Additionally, less than 1.00% of the dose was recovered from either urine or bile. 3. BS1801-related components were widely distributed throughout the body. 4. Fifteen metabolites were identified in rat plasma, urine, feces, and bile, and BS1801 was detected only in feces. 5. BS1801-M484, the methylation product obtained via a N–Se bond reduction in BS1801, was the most abundant drug-related component in plasma. The main metabolic pathways of BS1801 were reduction, amide hydrolysis, oxidation, and methylation. Overall, BS1801 was distributed throughout the body, and excreted mainly as an intact BS1801 form through feces. No differences were observed between male and female rats in distribution, metabolism, and excretion of BS1801.

Published

2023

222. In Silico and In Vivo Pharmacokinetic Evaluation of 84-B10, a Novel Drug Candidate against Acute Kidney Injury and Chronic Kidney Disease

Author

Man Su, Xianru Liu, Yuru Zhao, Yatong Zhu, Mengqiu Wu, Kun Liu, Gangqiang Yang, Wanhui Liu, and Lin Wang

Subjects

chronic kidney disease, 84-B10, pharmacokinetic, tissue distribution, physiologically based pharmacokinetic model, Organic chemistry, QD241-441

Abstract

Acute kidney injury (AKI) and chronic kidney disease (CKD) have become public health problems due to high morbidity and mortality. Currently, drugs recommended for patients with AKI or CKD are extremely limited, and candidates based on a new mechanism need to be explored. 84-B10 is a novel 3-phenylglutaric acid derivative that can activate the mitochondrial protease, Lon protease 1 (LONP1), and may protect against cisplatin-induced AKI and unilateral ureteral obstruction- or 5/6 nephrectomy [5/6Nx]-induced CKD model. Preclinical studies have shown that 84-B10 has a good therapeutic effect, low toxicity, and is a good prospect for further development. In the present study, the UHPLC-MS/MS method was first validated then applied to the pharmacokinetic study and tissue distribution of 84-B10 in rats. Physicochemical properties of 84-B10 were then acquired in silico. Based on these physicochemical and integral physiological parameters, a physiological based pharmacokinetic (PBPK) model was developed using the PK-Sim platform. The fitting accuracy was estimated with the obtained experimental data. Subsequently, the validated model was employed to predict the pharmacokinetic profiles in healthy and chronic kidney injury patients to evaluate potential clinical outcomes. Cmax in CKD patients was about 3250 ng/mL after a single dose of 84-B10 (0.41 mg/kg), and Cmax,ss was 1360 ng/mL after multiple doses. This study may serve in clinical dosage setting in the future.

Published

2023

223. Tissue Distribution, Pharmacokinetics, and Effect of Hematological and Biochemical Parameters of Acute Intravenous Administration of Silver Nanoparticles in Rats

Author

Elsayed I. Salim, Khaled Y. Abdel-Halim, Mostafa E. El-Mahalawy, Haitham A. Badr, and Hafiz Ahmed

Subjects

silver nanoparticles, pharmacokinetics, tissue distribution, hematological and biochemical alterations, rats, Chemistry, QD1-999

Abstract

The widespread biomedical and commercial applications of silver nanoparticles (AgNPs) have increased their potential for human and environmental exposure and toxicity to human health. The bio-distribution and toxicity of AgNPs in rodents following inhalation, intratracheal instillation, and oral ingestion are well documented; however, little is known about the bio-distribution of intravenously (IV)-administered AgNPs and their organ-specific pathophysiological effects. Here, we investigate the pharmacokinetic pattern and tissue distribution of AgNPs in male rats following IV administration. The animals were humanely sacrificed after 10 min, 1 h, 6 h, 12 h, 24 h, and 168 h of AgNP administration, and the silver (Ag) content was measured from blood samples and various tissues following acid digestion. The AgNPs were readily absorbed and subsequently distributed into most organs predominantly in the colon, small intestine, kidney, and heart after 6 h; however, they were the highest in the spinal cord after 168 h. White blood cells (WBCs) were significantly increased (42–60%) in AgNP-administered animals at all time points except 10 min. Regarding platelets, all AgNP-administered animals showed counts 7.8–39.2% lower, with the lowest count at 168 h post-administration. In the case of lymphocytes (LYMs), the AgNP-treated animals exhibited a count 19.5–41% lower at 10 min and 1 h post-administration; however, the animals at 168 h post-administration showed a count 30.5% more. The mean corpuscular hemoglobin (MCH) counts from the AgNP-treated animals were decreased by 50–62%. The concentrations of aspartate transaminase (AST), urea, and creatinine were increased in the AgNP-treated animals. Taken together, the results suggest that the acute IV administration of AgNPs alters metabolic and hematological parameters in animals and may pose a health risk to humans.

Published

2023

224. Pharmacokinetics, pharmacodynamics and safety studies on URB937, a peripherally restricted fatty acid amide hydrolase inhibitor, in rats

Author

Vozella, Valentina, Ahmed, Faizy, Choobchian, Paoula, Merrill, Collin B, Zibardi, Cristina, Tarzia, Giorgio, Mor, Marco, Duranti, Andrea, Tontini, Andrea, Rivara, Silvia, and Piomelli, Daniele

Subjects

Neurosciences, Development of treatments and therapeutic interventions, 6.1 Pharmaceuticals, Evaluation of treatments and therapeutic interventions, 5.1 Pharmaceuticals, Neurological, Oral and gastrointestinal, Administration, Oral, Amidohydrolases, Animals, Brain, Cannabinoids, Chromatography, Liquid, Dose-Response Relationship, Drug, Enzyme Inhibitors, Female, Male, Rats, Rats, Sprague-Dawley, Tandem Mass Spectrometry, Tissue Distribution, analgesia, endocannabinoid, fatty acid amide hydrolase, oleoylethanolamide, URB937, Pharmacology and Pharmaceutical Sciences, Medical Physiology, Pharmacology & Pharmacy

Abstract

ObjectivesURB937, a peripheral fatty acid amide hydrolase (FAAH) inhibitor, exerts profound analgesic effects in animal models. We examined, in rats, (1) the pharmacokinetic profile of oral URB937; (2) the compound's ability to elevate levels of the representative FAAH substrate, oleoylethanolamide (OEA); and (3) the compound's tolerability after oral administration.MethodsWe developed a liquid chromatography/tandem mass spectrometry (LC/MS-MS) method to measure URB937 and used a pre-existing LC/MS-MS assay to quantify OEA. FAAH activity was measured using a radioactive substrate. The tolerability of single or repeated (once daily for 2 weeks) oral administration of supramaximal doses of URB937 (100, 300, 1000 mg/kg) was assessed by monitoring food intake, water intake and body weight, followed by post-mortem evaluation of organ structure.Key findingsURB937 was orally available in male rats (F = 36%), but remained undetectable in brain when administered at doses that maximally inhibit FAAH activity and elevate OEA in plasma and liver. Acute and subchronic treatment with high doses of URB937 was well-tolerated and resulted in FAAH inhibition in brain.ConclusionsPain remains a major unmet medical need. The favourable pharmacokinetic and pharmacodynamic properties of URB937, along with its tolerability, encourage further development studies on this compound.

Published

2019

225. Safety, pharmacokinetics, and pharmacodynamic activity of obinutuzumab, a type 2 anti-CD20 monoclonal antibody for the desensitization of candidates for renal transplant

Author

Redfield, Robert R, Jordan, Stanley C, Busque, Stephan, Vincenti, Flavio, Woodle, E Steve, Desai, Niraj, Reed, Elaine F, Tremblay, Simon, Zachary, Andrea A, Vo, Ashley A, Formica, Richard, Schindler, Thomas, Tran, Ha, Looney, Caroline, Jamois, Candice, Green, Cherie, Morimoto, Alyssa, Rajwanshi, Richa, Schroeder, Aaron, Cascino, Matthew D, Brunetta, Paul, and Borie, Dominic

Subjects

Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Immunology, Kidney Disease, Patient Safety, Clinical Research, 6.1 Pharmaceuticals, Evaluation of treatments and therapeutic interventions, 6.2 Cellular and gene therapies, Renal and urogenital, Adolescent, Adult, Aged, Antibodies, Monoclonal, Humanized, Antigens, CD20, Antineoplastic Agents, Immunological, Cohort Studies, Desensitization, Immunologic, Female, Follow-Up Studies, Graft Survival, HLA Antigens, Humans, Kidney Failure, Chronic, Kidney Transplantation, Male, Maximum Tolerated Dose, Middle Aged, Patient Selection, Prognosis, Risk Factors, Tissue Distribution, Young Adult, alloantibody, B cell biology, clinical research, practice, clinical trial, immunosuppressant - fusion proteins and monoclonal antibodies, B cell specific, immunosuppression, immune modulation, kidney transplantation, nephrology, pharmacology, clinical research/practice, immunosuppressant - fusion proteins and monoclonal antibodies: B cell specific, immunosuppression/immune modulation, kidney transplantation/nephrology, Medical and Health Sciences, Surgery, Clinical sciences

Abstract

The limited effectiveness of rituximab plus intravenous immunoglobulin (IVIG) in desensitization may be due to incomplete B cell depletion. Obinutuzumab is a type 2 anti-CD20 antibody that induces increased B cell depletion relative to rituximab and may therefore be more effective for desensitization. This open-label phase 1b study assessed the safety, pharmacokinetics, and pharmacodynamics of obinutuzumab in highly sensitized patients with end-stage renal disease. Patients received 1 (day 1, n = 5) or 2 (days 1 and 15; n = 20) infusions of 1000-mg obinutuzumab followed by 2 doses of IVIG on days 22 and 43. Eleven patients received additional obinutuzumab doses at the time of transplant and/or at week 24. The median follow-up duration was 9.4 months. Obinutuzumab was well tolerated, and most adverse events were grade 1-2 in severity. There were 11 serious adverse events (SAEs) in 9 patients (36%); 10 of these SAEs were infections and 4 occurred after kidney transplant. Obinutuzumab plus IVIG resulted in profound peripheral B cell depletion and appeared to reduce B cells in retroperitoneal lymph nodes. Reductions in anti-HLA antibodies, number of unacceptable antigens, and the calculated panel reactive antibody score as centrally assessed using single-antigen bead assay were limited and not clinically meaningful for most patients (NCT02586051).

Published

2019

226. Octadecyloxyethyl benzyl tenofovir: A novel tenofovir diester provides sustained intracellular levels of tenofovir diphosphate

Author

Beadle, James R, Aldern, Kathy A, Zhang, Xing-Quan, Valiaeva, Nadejda, Hostetler, Karl Y, and Schooley, Robert T

Subjects

Medical Microbiology, Biomedical and Clinical Sciences, Immunology, Infectious Diseases, HIV/AIDS, Prevention, Infection, Adenine, Chemistry Techniques, Synthetic, Esters, Humans, Molecular Structure, Organophosphates, Tenofovir, Tissue Distribution, HIV-1 prophylaxis, Long-acting antiretroviral, Adherence, Microbiology, Pharmacology and Pharmaceutical Sciences, Virology, Medical microbiology, Pharmacology and pharmaceutical sciences

Abstract

Pre-exposure prophylaxis (PrEP) with topically or systemically administered antiretroviral agents can prevent acquisition of human immunodeficiency virus type 1 (HIV-1) infection. However, in clinical trials using tenofovir-containing agents, HIV-1 acquisition is reduced but not eliminated. Incomplete adherence remains the major contributor to failure. Sustained release or long-acting antiretroviral agents may provide better HIV-1 protection by reducing the clinical impact of incomplete adherence. To reduce dosing frequency, we synthesized a novel tenofovir prodrug, octadecyloxyethyl benzyl tenofovir (ODE-Bn-TFV), that is designed to release TFV slowly in tissues, and showed potent anti-HIV activity in vitro (EC50 = 1.7 nM). In cells exposed to 14C labeled TFV, ODE-Bn-TFV or the quickly activated monoester ODE-TFV, rapid cellular uptake for both lipophilic analogs was noted, achieving 50-fold higher levels than unmodified TFV after 48 h. Following exposure to ODE-[8-14C]TFV, the intracellular diphosphate levels were approximately four-fold higher than with ODE-Bn-TFV. However, intracellular TFVpp drug levels fell rapidly yielding a half-life of about two days. TFVpp levels in ODE-Bn-TFV treated cells decreased much more slowly and reached half-maximal levels in about seven days. These results suggest early accumulation of ODE-Bn-TFV followed by sustained intracellular release following cleavage of the ester bonds linking the ODE and benzyl moieties to the active molecular precursor, thereby potentially allowing for less frequent administration than with more rapidly activated forms of tenofovir.

Published

2019

227. How Transporters Have Changed Basic Pharmacokinetic Understanding

Author

Benet, Leslie Z, Bowman, Christine M, and Sodhi, Jasleen K

Subjects

Pharmacology and Pharmaceutical Sciences, Biomedical and Clinical Sciences, Patient Safety, Animals, Biological Availability, Drug Interactions, Humans, Membrane Transport Proteins, Metabolic Clearance Rate, Models, Biological, Pharmaceutical Preparations, Tissue Distribution, clearance, half-life, mean residence time, transporters, volume of distribution, Pharmacology & Pharmacy, Pharmacology and pharmaceutical sciences

Abstract

The emergence and continued evolution of the transporter field has caused re-evaluation and refinement of the original principles surrounding drug disposition. In this paper, we emphasize the impact that transporters can have on volume of distribution and how this can affect the other major pharmacokinetic parameters. When metabolic drug-drug interactions or pharmacogenomic variance changes the metabolism of a drug, the volume of distribution appears to be unchanged while clearance, bioavailability, and half-life are changed. When transporters are involved in the drug-drug interactions or pharmacogenomic variance, the volume of distribution can be markedly affected causing counterintuitive changes in half-life. Cases are examined where a volume of distribution change is significant enough that although clearance decreases, half-life decreases. Thus, drug dosing decisions must be made based on CL/F changes, not half-life changes, as such volume of distribution alterations will also influence the half-life results.

Published

2019

228. A Dual-Modality Linker Enables Site-Specific Conjugation of Antibody Fragments for 18F-Immuno-PET and Fluorescence Imaging

Author

Zettlitz, Kirstin A, Waldmann, Christopher M, Tsai, Wen-Ting K, Tavaré, Richard, Collins, Jeffrey, Murphy, Jennifer M, and Wu, Anna M

Subjects

Biomedical and Clinical Sciences, Clinical Sciences, Bioengineering, Biomedical Imaging, Cancer, Prostate Cancer, Biotechnology, Urologic Diseases, Animals, Antibodies, Antigens, Neoplasm, Carbocyanines, Cyclooctanes, Cysteine, Fluorescence, Fluorescent Dyes, Fluorine Radioisotopes, GPI-Linked Proteins, Humans, Immunoglobulin Fragments, Male, Mice, Microscopy, Fluorescence, Neoplasm Proteins, Neoplasm Transplantation, Optical Imaging, Positron-Emission Tomography, Prostatic Neoplasms, Radiopharmaceuticals, Tissue Distribution, immuno-PET, fluorescence image, guided surgery, cys-diabody, F-18, click chemistry, 18F, fluorescence image-guided surgery, Nuclear Medicine & Medical Imaging, Clinical sciences

Abstract

Antibody-based dual-modality (PET/fluorescence) imaging enables both presurgery antigen-specific immuno-PET for noninvasive whole-body evaluation and intraoperative fluorescence for visualization of superficial tissue layers for image-guided surgery. Methods: We developed a universal dual-modality linker (DML) that facilitates site-specific conjugation to a cysteine residue-bearing antibody fragment, introduction of a commercially available fluorescent dye (via an amine-reactive prosthetic group), and rapid and efficient radiolabeling via click chemistry with 18F-labeled trans-cyclooctene (18F-TCO). To generate a dual-modality antibody fragment-based imaging agent, the DML was labeled with the far-red dye sulfonate cyanine 5 (sCy5), site-specifically conjugated to the C-terminal cysteine of the anti-prostate stem cell antigen (PSCA) cys-diabody A2, and subsequently radiolabeled by click chemistry with 18F-TCO. The new imaging probe was evaluated in a human PSCA-positive prostate cancer xenograft model by sequential immuno-PET and optical imaging. Uptake in target tissues was confirmed by ex vivo biodistribution. Results: We successfully synthesized a DML for conjugation of a fluorescent dye and 18F. The anti-PSCA cys-diabody A2 was site-specifically conjugated with either DML or sCy5 and radiolabeled via click chemistry with 18F-TCO. Immuno-PET imaging confirmed in vivo antigen-specific targeting of prostate cancer xenografts as early as 1 h after injection. Rapid renal clearance of the 50-kDa antibody fragment enables same-day imaging. Optical imaging showed antigen-specific fluorescent signal in PSCA-positive xenografts and high contrast to surrounding tissue and PSCA-negative xenografts. Conclusion: The DML enables site-specific conjugation away from the antigen-binding site of antibody fragments, with a controlled linker-to-protein ratio, and combines signaling moieties for 2 imaging systems into 1 molecule. Dual-modality imaging could provide both noninvasive whole-body imaging with organ-level biodistribution and fluorescence image-guided identification of tumor margins during surgery.

Published

2019

229. Synthesis and Initial Biological Evaluation of Boron-Containing Prostate-Specific Membrane Antigen Ligands for Treatment of Prostate Cancer Using Boron Neutron Capture Therapy

Author

Wang, Sinan, Blaha, Charles, Santos, Raquel, Huynh, Tony, Hayes, Thomas R, Beckford-Vera, Denis R, Blecha, Joseph E, Hong, Andrew S, Fogarty, Miko, Hope, Thomas A, Raleigh, David R, Wilson, David M, Evans, Michael J, VanBrocklin, Henry F, Ozawa, Tomoko, and Flavell, Robert R

Subjects

Biomedical and Clinical Sciences, Clinical Sciences, Oncology and Carcinogenesis, Cancer, Urologic Diseases, Bioengineering, Prostate Cancer, Biomedical Imaging, Biotechnology, Aging, 5.1 Pharmaceuticals, Development of treatments and therapeutic interventions, Animals, Antigens, Surface, Boron Compounds, Boron Neutron Capture Therapy, Boronic Acids, Cell Line, Tumor, Cell Survival, Drug Delivery Systems, Edetic Acid, Gallium Isotopes, Gallium Radioisotopes, Glutamate Carboxypeptidase II, Humans, Inhibitory Concentration 50, Ligands, Male, Mice, Mice, Nude, Oligopeptides, Phenylalanine, Positron Emission Tomography Computed Tomography, Prostatic Neoplasms, Radiation-Sensitizing Agents, Tissue Distribution, Xenograft Model Antitumor Assays, boron neutron capture therapy, prostate cancer, prostate-specific membrane antigen (PSMA) inhibitor, carborane, boron uptake, Macromolecular and Materials Chemistry, Pharmacology and Pharmaceutical Sciences, Pharmacology & Pharmacy, Pharmacology and pharmaceutical sciences

Abstract

Boron neutron capture therapy (BNCT) is a therapeutic modality which has been used for the treatment of cancers, including brain and head and neck tumors. For effective treatment via BNCT, efficient and selective delivery of a high boron dose to cancer cells is needed. Prostate-specific membrane antigen (PSMA) is a target for prostate cancer imaging and drug delivery. In this study, we conjugated boronic acid or carborane functional groups to a well-established PSMA inhibitor scaffold to deliver boron to prostate cancer cells and prostate tumor xenograft models. Eight boron-containing PSMA inhibitors were synthesized. All of these compounds showed a strong binding affinity to PSMA in a competition radioligand binding assay (IC50 from 555.7 to 20.3 nM). Three selected compounds 1a, 1d, and 1f were administered to mice, and their in vivo blocking of 68Ga-PSMA-11 uptake was demonstrated through a positron emission tomography (PET) imaging and biodistribution experiment. Biodistribution analysis demonstrated boron uptake of 4-7 μg/g in 22Rv1 prostate xenograft tumors and similar tumor/muscle ratios compared to the ratio for the most commonly used BNCT compound, 4-borono-l-phenylalanine (BPA). Taken together, these data suggest a potential role for PSMA targeted BNCT agents in prostate cancer therapy following suitable optimization.

Published

2019

230. Endovascular Ion Exchange Chemofiltration Device Reduces Off-Target Doxorubicin Exposure in a Hepatic Intra-arterial Chemotherapy Model

Author

Yee, Colin, McCoy, David, Yu, Jay, Losey, Aaron, Jordan, Caroline, Moore, Terilyn, Stillson, Carol, Oh, Hee Jeung, Kilbride, Bridget, Roy, Shuvo, Patel, Anand, Wilson, Mark W, Hetts, Steven W, and Consortium, on behalf of the ChemoFilter

Subjects

Digestive Diseases, Cardiovascular, Rare Diseases, Liver Disease, Orphan Drug, Animals, Doxorubicin, Heart, Hepatic Artery, Infusions, Intra-Arterial, Ion Exchange, Liver, Swine, Tissue Distribution, ChemoFilter Consortium

Abstract

PurposeTo determine if endovascular chemofiltration with an ionic device (ChemoFilter [CF]) can be used to reduce systemic exposure and off-target biodistribution of doxorubicin (DOX) during hepatic intra-arterial chemotherapy (IAC) in a preclinical model.Materials and methodsHepatic IAC infusions were performed in six pigs with normal livers. Animals underwent two 10-minute intra-arterial infusions of DOX (200 mg) into the common hepatic artery. Both the treatment group and the control group received initial IAC at 0 minutes and a second dose at 200 minutes. Prior to the second dose, CF devices were deployed in and adjacent to the hepatic venous outflow tract of treatment animals. Systemic exposure to DOX was monitored via blood samples taken during IAC procedures. After euthanasia, organ tissue DOX concentrations were analyzed. Alterations in systemic DOX exposure and biodistribution were compared by using one-tailed t tests.ResultsCF devices were well tolerated, and no hemodynamic, thrombotic, or immunologic complications were observed. Animals treated with a CF device had a significant reduction in systemic exposure when compared with systemic exposure in the control group (P

Published

2019

231. Molecular Imaging of the Glomerulus via Mesangial Cell Uptake of Radiolabeled Tilmanocept

Author

Qin, Zhengtao, Hoh, Carl K, Olson, Emilia S, Jahromi, Amin Haghighat, Hall, David J, Barback, Christopher V, You, Young-Hyun, Yanagita, Motoko, Sharma, Kumar, and Vera, David R

Subjects

Biomedical and Clinical Sciences, Clinical Sciences, Biomedical Imaging, Kidney Disease, Renal and urogenital, Animals, Dextrans, Immunohistochemistry, Injections, Intravenous, Kidney Glomerulus, Kinetics, Lectins, C-Type, Liver, Lymph Nodes, Male, Mannose Receptor, Mannose-Binding Lectins, Mesangial Cells, Mice, Microscopy, Fluorescence, Molecular Imaging, Positron-Emission Tomography, Radiopharmaceuticals, Rats, Receptors, Cell Surface, Sentinel Lymph Node Biopsy, Technetium Tc 99m Pentetate, Tissue Distribution, Tomography, Emission-Computed, Single-Photon, Whole Body Imaging, kidney imaging, 99mTc-tilmanocept, Ga-68-tilmanocept, mesangial cells, 68Ga-tilmanocept, Nuclear Medicine & Medical Imaging, Clinical sciences

Abstract

An unmet need for the clinical management of chronic kidney disease is a predictive tool of kidney function during the first decade of the disease, when there is silent loss of glomerular function. The objective of this study was to demonstrate receptor-mediated binding of tilmanocept to CD206 within the kidney and provide evidence of kinetic sensitivity of this binding to renal function. Methods: Rats were positioned in a PET scanner with the liver and kidneys within the field of view. After an intravenous injection of 68Ga-IRDye800-tilmanocept, using 1 of 2 scaled molar doses (0.02 nmol/g, n = 5; or 0.10 nmol/g, n = 5), or coinjection (n = 3) of 68Ga-IRDye800-tilmanocept (0.10 nmol/g) and unlabeled tilmanocept (5.0 nmol/g), or a negative control, 68Ga-IRDye800-DTPA-galactosyl-dextran (0.02 nmol/g, n = 5), each animal was imaged for 20 min followed by a whole-body scan. Frozen kidney sections were stained for podocytes and CD206 using immunofluorescence. Molecular imaging of diabetic db/db mice (4.9 wk, n = 6; 7.3 wk, n = 4; 13.3 wk, n = 6) and nondiabetic db/m mice (n = 6) was performed with fluorescence-labeled 99mTc-tilmanocept (18.5 MBq, 2.6 nmol). Thirty minutes after injection, blood, liver, kidneys, and urine were assayed for radioactivity. Renal time-activity curves were generated. Results: Rat PET whole-body images and time-activity curves of 68Ga-IRDye800-tilmanocept demonstrated receptor-mediated renal accumulation with evidence of glomerular uptake. Activity within the renal cortex persisted during the 40-min study. Histologic examination demonstrated colocalization of CD206 and IRDye800-tilmanocept within the glomerulus. The glomerular accumulation of the coinjection and the negative control studies were significantly less than the CD206-targeted agent. The db/db mice displayed a multiphasic renal time-activity curve with high urinary bladder accumulation; the nondiabetic mice exhibited renal uptake curves dominated by a single phase with low bladder accumulation. Conclusion: This study demonstrated receptor-mediated binding to the glomerular mesangial cells and kinetic sensitivity of tilmanocept to chronic renal disease. Given the role of mesangial cells during the progression of diabetic nephropathy, PET or SPECT renal imaging with radiolabeled tilmanocept may provide a noninvasive quantitative assessment of glomerular function.

Published

2019

232. Safe and Sustained Expression of Human Iduronidase After Intrathecal Administration of Adeno-Associated Virus Serotype 9 in Infant Rhesus Monkeys

Author

Hordeaux, Juliette, Hinderer, Christian, Buza, Elizabeth L, Louboutin, Jean-Pierre, Jahan, Tahsin, Bell, Peter, Chichester, Jessica A, Tarantal, Alice F, and Wilson, James M

Subjects

Medical Biotechnology, Biomedical and Clinical Sciences, Digestive Diseases, Rare Diseases, Genetics, Neurosciences, Biotechnology, Pediatric, Gene Therapy, Neurodegenerative, Brain Disorders, Development of treatments and therapeutic interventions, 5.2 Cellular and gene therapies, Neurological, Animals, Dependovirus, Female, Ganglia, Spinal, Gene Expression, Gene Transfer Techniques, Genetic Therapy, Genetic Vectors, Humans, Iduronidase, Immunohistochemistry, Injections, Spinal, Macaca mulatta, Neurons, Organ Specificity, Promoter Regions, Genetic, Serogroup, Tissue Distribution, Transgenes, AAV9, intrathecal, MPS I, infant, rhesus monkey, Immunology, Medical biotechnology

Abstract

Many neuropathic diseases cause early, irreversible neurologic deterioration, which warrants therapeutic intervention during the first months of life. In the case of mucopolysaccharidosis type I, a recessive lysosomal storage disorder that results from a deficiency of the lysosomal enzyme α-l-iduronidase (IDUA), one of the most promising treatment approaches is to restore enzyme expression through gene therapy. Specifically, administering pantropic adeno-associated virus (AAV) encoding IDUA into the cerebrospinal fluid (CSF) via suboccipital administration has demonstrated remarkable efficacy in large animals. Preclinical safety studies conducted in adult nonhuman primates supported a positive risk-benefit profile of the procedure while highlighting potential subclinical toxicity to primary sensory neurons located in the dorsal root ganglia (DRG). This study investigated the long-term performance of intrathecal cervical AAV serotype 9 gene transfer of human IDUA administered to 1-month-old rhesus monkeys (N = 4) with half of the animals tolerized to the human transgene at birth via systemic administration of an AAV serotype 8 vector expressing human IDUA from the liver. Sustained expression of the transgene for almost 4 years is reported in all animals. Transduced cells were primarily pyramidal neurons in the cortex and hippocampus, Purkinje cells in the cerebellum, lower motor neurons, and DRG neurons. Both tolerized and non-tolerized animals were robust and maintained transgene expression as measured by immunohistochemical analysis of brain tissue. However, the presence of antibodies in the non-tolerized animals led to a loss of measurable levels of secreted enzyme in the CSF. These results support the safety and efficiency of treating neonatal rhesus monkeys with AAV serotype 9 gene therapy delivered into the CSF.

Published

2019

233. Antisense Oligonucleotide Therapies for Neurodegenerative Diseases

Author

Bennett, C Frank, Krainer, Adrian R, and Cleveland, Don W

Subjects

Pharmacology and Pharmaceutical Sciences, Biomedical and Clinical Sciences, Neurosciences, Neurodegenerative, Huntington's Disease, Biotechnology, Orphan Drug, Rare Diseases, Brain Disorders, Development of treatments and therapeutic interventions, 5.1 Pharmaceuticals, Neurological, Good Health and Well Being, Animals, Brain, Humans, Muscular Atrophy, Spinal, Neurodegenerative Diseases, Oligonucleotides, Oligonucleotides, Antisense, Tissue Distribution, amyotrophic lateral sclerosis, antisense oligonucleotides, Huntington's disease, RNA, spinal muscular atrophy, Psychology, Cognitive Sciences, Neurology & Neurosurgery, Biological psychology

Abstract

Antisense oligonucleotides represent a novel therapeutic platform for the discovery of medicines that have the potential to treat most neurodegenerative diseases. Antisense drugs are currently in development for the treatment of amyotrophic lateral sclerosis, Huntington's disease, and Alzheimer's disease, and multiple research programs are underway for additional neurodegenerative diseases. One antisense drug, nusinersen, has been approved for the treatment of spinal muscular atrophy. Importantly, nusinersen improves disease symptoms when administered to symptomatic patients rather than just slowing the progression of the disease. In addition to the benefit to spinal muscular atrophy patients, there are discoveries from nusinersen that can be applied to other neurological diseases, including method of delivery, doses, tolerability of intrathecally delivered antisense drugs, and the biodistribution of intrathecal dosed antisense drugs. Based in part on the early success of nusinersen, antisense drugs hold great promise as a therapeutic platform for the treatment of neurological diseases.

Published

2019

234. Phase I Study of CTT1057, an 18F-Labeled Imaging Agent with Phosphoramidate Core Targeting Prostate-Specific Membrane Antigen in Prostate Cancer

Author

Behr, Spencer C, Aggarwal, Rahul, VanBrocklin, Henry F, Flavell, Robert R, Gao, Kenneth, Small, Eric J, Blecha, Joseph, Jivan, Salma, Hope, Thomas A, Simko, Jeffry P, Kurhanewicz, John, Noworolski, Susan M, Korn, Natalie J, De Los Santos, Romelyn, Cooperberg, Matthew R, Carroll, Peter R, Nguyen, Hao G, Greene, Kirsten L, Langton-Webster, Beatrice, Berkman, Clifford E, and Seo, Youngho

Subjects

Biomedical and Clinical Sciences, Clinical Sciences, Oncology and Carcinogenesis, Clinical Research, Biomedical Imaging, Bioengineering, Prostate Cancer, Urologic Diseases, Cancer, Aged, Amides, Antigens, Surface, Cohort Studies, Fluorine Radioisotopes, Glutamate Carboxypeptidase II, Humans, Isotope Labeling, Male, Middle Aged, Phosphoric Acids, Positron-Emission Tomography, Prospective Studies, Prostatic Neoplasms, Safety, Tissue Distribution, Whole Body Imaging, prostate cancer, PSMA, PET, dosimetry, CTT1057, Nuclear Medicine & Medical Imaging, Clinical sciences

Abstract

Agents targeting prostate-specific membrane antigen (PSMA) comprise a rapidly emerging class of radiopharmaceuticals for diagnostic imaging of prostate cancer. Unlike most other PSMA agents with a urea backbone, CTT1057 is based on a phosphoramidate scaffold that irreversibly binds to PSMA. We conducted a first-in-humans phase I study of CTT1057 in patients with localized and metastatic prostate cancer. Methods: Two patient cohorts were recruited. Cohort A patients had biopsy-proven localized prostate cancer preceding radical prostatectomy, and cohort B patients had metastatic castration-resistant prostate cancer. Cohort A patients were imaged at multiple time points after intravenous injection with 362 ± 8 MBq of CTT1057 to evaluate the kinetics of CTT1057 and estimate radiation dose profiles. Mean organ-absorbed doses and effective doses were calculated. CTT1057 uptake in the prostate gland and regional lymph nodes was correlated with pathology, PSMA staining, and the results of conventional imaging. In cohort B, patients were imaged 60-120 min after injection of CTT1057. PET images were assessed for overall image quality, and areas of abnormal uptake were contrasted with conventional imaging. Results: In cohort A (n = 5), the average total effective dose was 0.023 mSv/MBq. The kidneys exhibited the highest absorbed dose, 0.067 mGy/MBq. The absorbed dose of the salivary glands was 0.015 mGy/MBq. For cohort B (n = 15), CTT1057 PET detected 97 metastatic lesions, and 44 of 56 bone metastases detected on CTT1057 PET (78.5%) were also detectable on bone scanning. Eight of 32 lymph nodes positive on CTT1057 PET (25%) were enlarged by size criteria on CT. Conclusion: CTT1057 is a promising novel phosphoramidate PSMA-targeting 18F-labeled PET radiopharmaceutical that demonstrates similar biodistribution to urea-based PSMA-targeted agents, with lower exposure to the kidneys and salivary glands. Metastatic lesions are detected with higher sensitivity on CTT1057 imaging than on conventional imaging. Further prospective studies with CTT1057 are warranted to elucidate its role in cancer imaging.

Published

2019

235. Creatine based polymer for codelivery of bioengineered MicroRNA and chemodrugs against breast cancer lung metastasis

Author

Xu, Jieni, Sun, Jingjing, Ho, Pui Yan, Luo, Zhangyi, Ma, Weina, Zhao, Wenchen, Rathod, Sanjay B, Fernandez, Christian A, Venkataramanan, Raman, Xie, Wen, Yu, Ai-Ming, and Li, Song

Subjects

Biomedical and Clinical Sciences, Medicinal and Biomolecular Chemistry, Chemical Sciences, Oncology and Carcinogenesis, Genetics, Bioengineering, Breast Cancer, Lung Cancer, Lung, Cancer, Biotechnology, Development of treatments and therapeutic interventions, 5.1 Pharmaceuticals, 5.2 Cellular and gene therapies, Animals, Antineoplastic Agents, Breast Neoplasms, Cell Line, Tumor, Creatine, Down-Regulation, Drug Delivery Systems, Endocytosis, Female, Humans, Lung Neoplasms, Mice, Inbred BALB C, Micelles, MicroRNAs, Nanoparticles, Polymers, Tissue Distribution, Cancer metastasis, Multifunctional nanocarriers, Chemo-gene combination therapy, Bioengineered miRNA prodrug

Abstract

Metastasis is the major cause for breast cancer related mortality. The combination of miRNA-based therapy and chemotherapy represents a promising approach against breast cancer lung metastasis. The goal of this study is to develop an improved therapy that co-delivers a novel bioengineered miRNA prodrug (tRNA-mir-34a) and doxorubicin (DOX) via a multifunctional nanomicellar carrier that is based on a conjugate of amphiphilic copolymer POEG-VBC backbone with creatine, a naturally occurring cationic molecule. Co-delivery of DOX leads to more effective processing of tRNA-mir-34a into mature miR-34a and down-regulation of target genes. DOX + tRNA-mir-34a/POEG-PCre exhibits potent synergistic anti-tumor and anti-metastasis activity in vitro and in vivo. Interestingly, the enhanced immune response contributes to the overall antitumor efficacy. POEG-PCre may represent a safe and effective delivery system for an optimal chemo-gene combination therapy.

Published

2019

236. An Open‐Label, Multicenter, Phase I, Dose Escalation Study with Phase II Expansion Cohort to Determine the Safety, Pharmacokinetics, and Preliminary Antitumor Activity of Intravenous TKM‐080301 in Subjects with Advanced Hepatocellular Carcinoma

Author

Dika, Imane El, Lim, Ho Yeong, Yong, Wei Peng, Lin, Chia‐Chi, Yoon, Jung‐Hwan, Modiano, Manuel, Freilich, Bradley, Choi, Hye Jin, Chao, Tsu‐Yi, Kelley, Robin K, Brown, Joanne, Knox, Jennifer, Ryoo, Baek‐Yeol, Yau, Thomas, and Abou‐Alfa, Ghassan K

Subjects

Biomedical and Clinical Sciences, Clinical Sciences, Oncology and Carcinogenesis, Genetics, Clinical Trials and Supportive Activities, Liver Disease, Digestive Diseases, Cancer, Rare Diseases, Clinical Research, Liver Cancer, 6.1 Pharmaceuticals, Evaluation of treatments and therapeutic interventions, Administration, Intravenous, Adult, Aged, Antineoplastic Agents, Carcinoma, Hepatocellular, Cohort Studies, Dose-Response Relationship, Drug, Female, Follow-Up Studies, Humans, Lipids, Liver Neoplasms, Male, Maximum Tolerated Dose, Middle Aged, Nanoparticles, Patient Safety, Prognosis, RNA, Small Interfering, Tissue Distribution, Oncology & Carcinogenesis, Oncology and carcinogenesis

Abstract

Lessons learnedTKM-080301 showed a favorable toxicity profile at the studied dose.TKM-080301 targeting PLK1 through small interfering RNA mechanism did not demonstrate improved overall survival in patients with advanced hepatocellular carcinoma compared with historical control. Preliminary antitumor activity as shown in this early-phase study does not support further evaluation as a single agent.BackgroundPolo-like kinase 1 (PLK1) is overexpressed in hepatocellular carcinoma (HCC). Knockdown of PLK1 expression by PLK1 small interfering RNA (siRNA) in an HCC cell line showed reduced expression in RNA-induced silencing complex and a reduction in cell proliferation.MethodsA 3 + 3 dose escalation plus expansion cohort at the maximum tolerated dose (MTD) was implemented. Patients with HCC, Eastern Cooperative Oncology Group (ECOG) performance status ≤2, and Child-Pugh score A received TKM-080301 as an intravenous infusion once every week for 3 consecutive weeks, repeated every 28 days.ResultsThe study enrolled 43 patients. The starting dose of TKM-080301 was 0.3 mg/kg, and MTD was declared at 0.75 mg/kg. Following the development of grade 4 thrombocytopenia in two subjects on the expansion cohort, the MTD was redefined at 0.6 mg/kg. Four patients did not have any evaluable postbaseline scan. Of the other 39 subjects who had received at least 0.3 mg/kg, 18 subjects (46.2%) had stable disease (SD) by independent RECIST 1.1 criteria. By Choi criteria, eight subjects (23.1%) had a partial response (PR). For 37 assessable subjects, with 2 subjects censored, median progression-free survival (PFS) was 2.04 months. Median survival for the whole study population was 7.5 months.ConclusionTKM-080301 was generally well tolerated. In this early-phase study, antitumor effect for TKM 080301 was limited. Further evaluation as a single agent in large randomized trials is not warranted.

Published

2019

237. An Open-Label, Multicenter, Phase I, Dose Escalation Study with Phase II Expansion Cohort to Determine the Safety, Pharmacokinetics, and Preliminary Antitumor Activity of Intravenous TKM-080301 in Subjects with Advanced Hepatocellular Carcinoma.

Author

El Dika, Imane, Lim, Ho Yeong, Yong, Wei Peng, Lin, Chia-Chi, Yoon, Jung-Hwan, Modiano, Manuel, Freilich, Bradley, Choi, Hye Jin, Chao, Tsu-Yi, Kelley, Robin K, Brown, Joanne, Knox, Jennifer, Ryoo, Baek-Yeol, Yau, Thomas, and Abou-Alfa, Ghassan K

Subjects

Humans, Carcinoma, Hepatocellular, Liver Neoplasms, Lipids, RNA, Small Interfering, Antineoplastic Agents, Prognosis, Cohort Studies, Follow-Up Studies, Maximum Tolerated Dose, Tissue Distribution, Dose-Response Relationship, Drug, Adult, Aged, Middle Aged, Female, Male, Nanoparticles, Patient Safety, Administration, Intravenous, Carcinoma, Hepatocellular, Dose-Response Relationship, Drug, Administration, Intravenous, Oncology and Carcinogenesis, Oncology & Carcinogenesis

Abstract

Lessons learnedTKM-080301 showed a favorable toxicity profile at the studied dose.TKM-080301 targeting PLK1 through small interfering RNA mechanism did not demonstrate improved overall survival in patients with advanced hepatocellular carcinoma compared with historical control. Preliminary antitumor activity as shown in this early-phase study does not support further evaluation as a single agent.BackgroundPolo-like kinase 1 (PLK1) is overexpressed in hepatocellular carcinoma (HCC). Knockdown of PLK1 expression by PLK1 small interfering RNA (siRNA) in an HCC cell line showed reduced expression in RNA-induced silencing complex and a reduction in cell proliferation.MethodsA 3 + 3 dose escalation plus expansion cohort at the maximum tolerated dose (MTD) was implemented. Patients with HCC, Eastern Cooperative Oncology Group (ECOG) performance status ≤2, and Child-Pugh score A received TKM-080301 as an intravenous infusion once every week for 3 consecutive weeks, repeated every 28 days.ResultsThe study enrolled 43 patients. The starting dose of TKM-080301 was 0.3 mg/kg, and MTD was declared at 0.75 mg/kg. Following the development of grade 4 thrombocytopenia in two subjects on the expansion cohort, the MTD was redefined at 0.6 mg/kg. Four patients did not have any evaluable postbaseline scan. Of the other 39 subjects who had received at least 0.3 mg/kg, 18 subjects (46.2%) had stable disease (SD) by independent RECIST 1.1 criteria. By Choi criteria, eight subjects (23.1%) had a partial response (PR). For 37 assessable subjects, with 2 subjects censored, median progression-free survival (PFS) was 2.04 months. Median survival for the whole study population was 7.5 months.ConclusionTKM-080301 was generally well tolerated. In this early-phase study, antitumor effect for TKM 080301 was limited. Further evaluation as a single agent in large randomized trials is not warranted.

Published

2019

238. Biodistribution and toxicological evaluation of micron- and nano-sized erythrocyte-derived optical particles in healthy Swiss Webster mice

Author

Vankayala, Raviraj, Mac, Jenny T, Burns, Joshua M, Dunn, Eugene, Carroll, Stefanie, Bahena, Edver M, Patel, Dipti K, Griffey, Stephen, and Anvari, Bahman

Subjects

Bioengineering, Nanotechnology, Digestive Diseases, Animals, Drug Carriers, Erythrocytes, Female, Indocyanine Green, Mice, Microspheres, Nanoparticles, Optical Imaging, Optical Phenomena, Tissue Distribution, Medicinal and Biomolecular Chemistry, Biochemistry and Cell Biology, Medical Biotechnology

Abstract

Particle-based systems provide a capability for the delivery of imaging and/or therapeutic payloads. We have engineered constructs derived from erythrocytes, and doped with the FDA-approved near infrared dye, indocyanine green (ICG). We refer to these optical particles as NIR erythrocyte-mimicking transducers (NETs). A particular feature of NETs is that their diameters can be tuned from micron- to nano-scale. Herein, we investigated the effects of micron- (≈2.6 μm diameter), and nano- (≈145 nm diameter) sized NETs on their biodistribution, and evaluated their acute toxicity in healthy Swiss Webster mice. Following tail vein injection of free ICG and NETs, animals were euthanized at various time points up to 48 hours. Fluorescence analysis of blood showed that nearly 11% of the injected amount of nano-sized NETs (nNETs) remained in blood at 48 hours post-injection as compared to ≈5% for micron-sized NETs (μNETs). Similarly, at this time point, higher levels of nNETs were present in various organs including the lungs, liver, and spleen. Histological analyses of various organs, extracted at 24 hours post-injection of NETs, did not show pathological alterations. Serum biochemistry profiles, in general, did not show elevated levels of the various analyzed biomarkers associated with liver and kidney functions. Values of various hematological profiles remained within the normal ranges following the administration of μNETs and nNETs. Results of this study suggest that erythrocyte-derived particles can potentially provide a non-toxic platform for delivery of ICG.

Published

2019

239. The Pediatric Cell Atlas: Defining the Growth Phase of Human Development at Single-Cell Resolution.

Author

Taylor, Deanne, Aronow, Bruce, Tan, Kai, Bernt, Kathrin, Salomonis, Nathan, Greene, Casey, Frolova, Alina, Henrickson, Sarah, Wells, Andrew, Pei, Liming, Jaiswal, Jyoti, Whitsett, Jeffrey, Hamilton, Kathryn, MacParland, Sonya, Kelsen, Judith, Heuckeroth, Robert, Potter, S, Vella, Laura, Terry, Natalie, Ghanem, Louis, Kennedy, Benjamin, Helbig, Ingo, Sullivan, Kathleen, Castelo-Soccio, Leslie, Kreigstein, Arnold, Herse, Florian, Nawijn, Martijn, Koppelman, Gerard, Haendel, Melissa, Harris, Nomi, Rokita, Jo, Zhang, Yuanchao, Regev, Aviv, Rozenblatt-Rosen, Orit, Rood, Jennifer, Tickle, Timothy, Vento-Tormo, Roser, Alimohamed, Saif, Lek, Monkol, Mar, Jessica, Loomes, Kathleen, Barrett, David, Uapinyoying, Prech, Beggs, Alan, Agrawal, Pankaj, Chen, Yi-Wen, Muir, Amanda, Garmire, Lana, Snapper, Scott, Nazarian, Javad, Seeholzer, Steven, Fazelinia, Hossein, Singh, Larry, Faryabi, Robert, Raman, Pichai, Dawany, Noor, Xie, Hongbo, Devkota, Batsal, Diskin, Sharon, Anderson, Stewart, Rappaport, Eric, Peranteau, William, Wikenheiser-Brokamp, Kathryn, Teichmann, Sarah, Wallace, Douglas, Peng, Tao, Ding, Yang-Yang, Kim, Man, Xing, Yi, Kong, Sek, Bönnemann, Carsten, Mandl, Kenneth, and White, Peter

Subjects

Embryonic Development, Gene Expression Profiling, Gene Expression Regulation, Developmental, Gene Regulatory Networks, Humans, Pediatrics, Single-Cell Analysis, Tissue Distribution

Abstract

Single-cell gene expression analyses of mammalian tissues have uncovered profound stage-specific molecular regulatory phenomena that have changed the understanding of unique cell types and signaling pathways critical for lineage determination, morphogenesis, and growth. We discuss here the case for a Pediatric Cell Atlas as part of the Human Cell Atlas consortium to provide single-cell profiles and spatial characterization of gene expression across human tissues and organs. Such data will complement adult and developmentally focused HCA projects to provide a rich cytogenomic framework for understanding not only pediatric health and disease but also environmental and genetic impacts across the human lifespan.

Published

2019

240. Tuberculosis drugs' distribution and emergence of resistance in patient's lung lesions: A mechanistic model and tool for regimen and dose optimization.

Author

Strydom, Natasha, Gupta, Sneha V, Fox, William S, Via, Laura E, Bang, Hyeeun, Lee, Myungsun, Eum, Seokyong, Shim, TaeSun, Barry, Clifton E, Zimmerman, Matthew, Dartois, Véronique, and Savic, Radojka M

Subjects

Lung, Humans, Tuberculosis, Multidrug-Resistant, Tuberculosis, Pulmonary, Disease Progression, Isoniazid, Pyrazinamide, Rifampin, Kanamycin, Antitubercular Agents, Treatment Failure, Drug Therapy, Combination, Drug Administration Schedule, Retrospective Studies, Drug Resistance, Multiple, Bacterial, Tissue Distribution, Decision Support Techniques, Adult, Middle Aged, Female, Male, Drug Dosage Calculations, Young Adult, Linezolid, General & Internal Medicine, Medical and Health Sciences

Abstract

BackgroundThe sites of mycobacterial infection in the lungs of tuberculosis (TB) patients have complex structures and poor vascularization, which obstructs drug distribution to these hard-to-reach and hard-to-treat disease sites, further leading to suboptimal drug concentrations, resulting in compromised TB treatment response and resistance development. Quantifying lesion-specific drug uptake and pharmacokinetics (PKs) in TB patients is necessary to optimize treatment regimens at all infection sites, to identify patients at risk, to improve existing regimens, and to advance development of novel regimens. Using drug-level data in plasma and from 9 distinct pulmonary lesion types (vascular, avascular, and mixed) obtained from 15 hard-to-treat TB patients who failed TB treatments and therefore underwent lung resection surgery, we quantified the distribution and the penetration of 7 major TB drugs at these sites, and we provide novel tools for treatment optimization.Methods and findingsA total of 329 plasma- and 1,362 tissue-specific drug concentrations from 9 distinct lung lesion types were obtained according to optimal PK sampling schema from 15 patients (10 men, 5 women, aged 23 to 58) undergoing lung resection surgery (clinical study NCT00816426 performed in South Korea between 9 June 2010 and 24 June 2014). Seven major TB drugs (rifampin [RIF], isoniazid [INH], linezolid [LZD], moxifloxacin [MFX], clofazimine [CFZ], pyrazinamide [PZA], and kanamycin [KAN]) were quantified. We developed and evaluated a site-of-action mechanistic PK model using nonlinear mixed effects methodology. We quantified population- and patient-specific lesion/plasma ratios (RPLs), dynamics, and variability of drug uptake into each lesion for each drug. CFZ and MFX had higher drug exposures in lesions compared to plasma (median RPL 2.37, range across lesions 1.26-22.03); RIF, PZA, and LZD showed moderate yet suboptimal lesion penetration (median RPL 0.61, range 0.21-2.4), while INH and KAN showed poor tissue penetration (median RPL 0.4, range 0.03-0.73). Stochastic PK/pharmacodynamic (PD) simulations were carried out to evaluate current regimen combinations and dosing guidelines in distinct patient strata. Patients receiving standard doses of RIF and INH, who are of the lower range of exposure distribution, spent substantial periods (>12 h/d) below effective concentrations in hard-to-treat lesions, such as caseous lesions and cavities. Standard doses of INH (300 mg) and KAN (1,000 mg) did not reach therapeutic thresholds in most lesions for a majority of the population. Drugs and doses that did reach target exposure in most subjects include 400 mg MFX and 100 mg CFZ. Patients with cavitary lesions, irrespective of drug choice, have an increased likelihood of subtherapeutic concentrations, leading to a higher risk of resistance acquisition while on treatment. A limitation of this study was the small sample size of 15 patients, performed in a unique study population of TB patients who failed treatment and underwent lung resection surgery. These results still need further exploration and validation in larger and more diverse cohorts.ConclusionsOur results suggest that the ability to reach and maintain therapeutic concentrations is both lesion and drug specific, indicating that stratifying patients based on disease extent, lesion types, and individual drug-susceptibility profiles may eventually be useful for guiding the selection of patient-tailored drug regimens and may lead to improved TB treatment outcomes. We provide a web-based tool to further explore this model and results at http://saviclab.org/tb-lesion/.

Published

2019

241. Identification of Factors Complicating Bioluminescence Imaging

Author

Yeh, Hsien-Wei, Wu, Tianchen, Chen, Minghai, and Ai, Hui-wang

Subjects

Genetics, Biomedical Imaging, Adenosine Triphosphate, Animals, Enzyme Stability, Genes, Reporter, HEK293 Cells, HeLa Cells, Humans, Imidazoles, Luciferases, Luminescent Agents, Luminescent Measurements, Mice, Inbred BALB C, Neoplasms, Pyrazines, Tissue Distribution, Hela Cells, Medicinal and Biomolecular Chemistry, Biochemistry and Cell Biology, Medical Biochemistry and Metabolomics, Biochemistry & Molecular Biology

Abstract

In vivo bioluminescence imaging (BLI) has become a standard, non-invasive imaging modality for following gene expression or the fate of proteins and cells in living animals. Currently, bioluminescent reporters used in laboratories are mostly derivatives of two major luciferase families: ATP-dependent insect luciferases and ATP-independent marine luciferases. Inconsistent results of experiments using different bioluminescent reporters, such as Akaluc and Antareas2, have been reported. Herein, we re-examined the inconsistency in several experimental settings and identified the factors, such as ATP dependency, stability in serum, and molecular sizes of luciferases, that contributed to the observed differences. We expect this study will make the research community aware of these factors and facilitate more accurate interpretation of BLI data by considering the nature of each bioluminescent reporter.

Published

2019

242. Gene Expression Networks Across Multiple Tissues Are Associated with Rates of Molecular Evolution in Wild House Mice.

Author

Mack, Katya L, Phifer-Rixey, Megan, Harr, Bettina, and Nachman, Michael W

Subjects

Animals, Mice, Gene Expression Profiling, Sequence Analysis, RNA, Genomics, Evolution, Molecular, Organ Specificity, Gene Expression Regulation, Tissue Distribution, Gene Regulatory Networks, Selection, Genetic, co-expression, gene regulation, house mice, Evolution, Molecular, Selection, Genetic, Sequence Analysis, RNA, Genetics

Abstract

Interactions between genes can influence how selection acts on sequence variation. In gene regulatory networks, genes that affect the expression of many other genes may be under stronger evolutionary constraint than genes whose expression affects fewer partners. While this has been studied for individual tissue types, we know less about the effects of regulatory networks on gene evolution across different tissue types. We use RNA-sequencing and genomic data collected from Mus musculus domesticus to construct and compare gene co-expression networks for 10 tissue types. We identify tissue-specific expression and local regulatory variation, and we associate these components of gene expression variation with sequence polymorphism and divergence. We found that genes with higher connectivity across tissues and genes associated with a greater number of cross-tissue modules showed significantly lower genetic diversity and lower rates of protein evolution. Consistent with this pattern, "hub" genes across multiple tissues also showed evidence of greater evolutionary constraint. Using allele-specific expression, we found that genes with cis-regulatory variation had lower average connectivity and higher levels of tissue specificity. Taken together, these results are consistent with strong purifying selection acting on genes with high connectivity within and across tissues.

Published

2019

243. Antiretroviral Concentrations in Hair Strongly Predict Virologic Response in a Large Human Immunodeficiency Virus Treatment-naive Clinical Trial

Author

Gandhi, Monica, Bacchetti, Peter, Ofokotun, Igho, Jin, Chengshi, Ribaudo, Heather J, Haas, David W, Sheth, Anandi N, Horng, Howard, Phung, Nhi, Kuncze, Karen, Okochi, Hideaki, Landovitz, Raphael J, Lennox, Jeffrey, Currier, Judith S, and Team, AIDS Clinical Trials Group 5257 Study

Subjects

Medical Microbiology, Biomedical and Clinical Sciences, Immunology, Clinical Research, Infectious Diseases, Clinical Trials and Supportive Activities, HIV/AIDS, Sexually Transmitted Infections, 6.1 Pharmaceuticals, Evaluation of treatments and therapeutic interventions, Infection, Good Health and Well Being, Adolescent, Adult, Aged, Anti-HIV Agents, Antiretroviral Therapy, Highly Active, Female, HIV Infections, HIV-1, Hair, Humans, Male, Middle Aged, Randomized Controlled Trials as Topic, Tissue Distribution, Treatment Failure, Treatment Outcome, Viral Load, Young Adult, HIV, A5257 study, AIDS Clinical Trials Group, hair concentrations, non-NNRTI regimens, AIDS Clinical Trials Group (ACTG) 5257 Study Team, Biological Sciences, Medical and Health Sciences, Microbiology, Clinical sciences

Abstract

Concentrations of antiretrovirals in hair are associated with virologic outcomes in cohorts of human immunodeficiency virus (HIV)-positive individuals but have never been examined in a clinical trial. We show for the first time the predictive utility of hair antiretroviral concentrations in a large HIV treatment-naive trial (AIDS Clinical Trials Group protocol A5257).

Published

2019

244. A Phase I/Ib Trial of the VEGFR-Sparing Multikinase RET Inhibitor RXDX-105

Author

Drilon, Alexander, Fu, Siqing, Patel, Manish R, Fakih, Marwan, Wang, Ding, Olszanski, Anthony J, Morgensztern, Daniel, Liu, Stephen V, Cho, Byoung Chul, Bazhenova, Lyudmila, Rodriguez, Cristina P, Doebele, Robert C, Wozniak, Antoinette, Reckamp, Karen L, Seery, Tara, Nikolinakos, Petros, Hu, Zheyi, Oliver, Jennifer W, Trone, Denise, McArthur, Katherine, Patel, Rupal, Multani, Pratik S, and Ahn, Myung-Ju

Subjects

Biomedical and Clinical Sciences, Clinical Sciences, Oncology and Carcinogenesis, Lung Cancer, Cancer, Clinical Research, Lung, Adult, Aged, Aged, 80 and over, Dose-Response Relationship, Drug, Female, Humans, Male, Middle Aged, Neoplasms, Oncogene Proteins, Fusion, Patient Safety, Phenylurea Compounds, Protein Kinase Inhibitors, Proto-Oncogene Proteins c-ret, Quinazolines, Tissue Distribution, Treatment Outcome, Vascular Endothelial Growth Factor Receptor-1, Biochemistry and cell biology, Oncology and carcinogenesis

Abstract

RET fusions are oncogenic drivers of various tumors, including non-small cell lung cancers (NSCLC). The safety and antitumor activity of the multikinase RET inhibitor RXDX-105 were explored in a phase I/Ib trial. A recommended phase II dose of 275 mg fed daily was identified. The most common treatment-related adverse events were fatigue (25%), diarrhea (24%), hypophosphatemia (18%), maculopapular rash (18%), and nonmaculopapular rash (17%). In the phase Ib cohort of RET inhibitor-naïve patients with RET fusion-positive NSCLCs, the objective response rate (ORR) was 19% (95% CI, 8%-38%, n = 6/31). Interestingly, the ORR varied significantly by the gene fusion partner (P < 0.001, Fisher exact test): 0% (95% CI, 0%-17%, n = 0/20) with KIF5B (the most common upstream partner for RET fusion-positive NSCLC), and 67% (95% CI, 30%-93%, n = 6/9) with non-KIF5B partners. The median duration of response in all RET fusion-positive NSCLCs was not reached (range, 5 to 18+ months). SIGNIFICANCE: Although KIF5B-RET is the most common RET fusion in NSCLCs, RET inhibition with RXDX-105 resulted in responses only in non-KIF5B-RET-containing cancers. Novel approaches to targeting KIF5B-RET-containing tumors are needed, along with a deeper understanding of the biology that underlies the differential responses observed.This article is highlighted in the In This Issue feature, p. 305.

Published

2019

245. In vitro and in vivo phasor analysis of stoichiometry and pharmacokinetics using short‐lifetime near‐infrared dyes and time‐gated imaging

Author

Chen, Sez‐Jade, Sinsuebphon, Nattawut, Rudkouskaya, Alena, Barroso, Margarida, Intes, Xavier, and Michalet, Xavier

Subjects

Biomedical Imaging, Bioengineering, Generic health relevance, Animals, Cell Line, Tumor, Coloring Agents, Fluorescence Resonance Energy Transfer, Humans, Immunoglobulin G, Infrared Rays, Mice, Optical Imaging, Receptors, Transferrin, Tissue Distribution, Transferrin, binding equilibrium, fluorescence, FRET, in vivo, lifetime, mouse, near-infrared, pharmacokinetics, phasor, transferrin, Optical Physics, Medicinal and Biomolecular Chemistry, Medical Biotechnology, Optoelectronics & Photonics

Abstract

We introduce a simple new approach for time-resolved multiplexed analysis of complex systems using near-infrared (NIR) dyes, applicable to in vitro and in vivo studies. We show that fast and precise in vitro quantification of NIR fluorophores' short (subnanosecond) lifetime and stoichiometry can be done using phasor analysis, a computationally efficient and user-friendly representation of complex fluorescence intensity decays obtained with pulsed laser excitation and time-gated camera imaging. We apply this approach to the study of binding equilibria by Förster resonant energy transfer using two different model systems: primary/secondary antibody binding in vitro and ligand/receptor binding in cell cultures. We then extend it to dynamic imaging of the pharmacokinetics of transferrin engagement with the transferrin receptor in live mice, elucidating the kinetics of differential transferrin accumulation in specific organs, straightforwardly differentiating specific from nonspecific binding. Our method, implemented in a freely-available software, has the advantage of time-resolved NIR imaging, including better tissue penetration and background-free imaging, but simplifies and considerably speeds up data processing and interpretation, while remaining quantitative. These advances make this method attractive and of broad applicability for in vitro and in vivo molecular imaging and could be extended to applications as diverse as image-guided surgery or optical tomography.

Published

2019

246. Phase 1 dose-escalation study of momelotinib, a Janus kinase 1/2 inhibitor, combined with gemcitabine and nab-paclitaxel in patients with previously untreated metastatic pancreatic ductal adenocarcinoma

Author

Ng, Kimmie, Hendifar, Andrew, Starodub, Alexander, Chaves, Jorge, Yang, Yingsi, Koh, Brian, Barbie, David, Hahn, William C, and Fuchs, Charles S

Subjects

Biomedical and Clinical Sciences, Clinical Sciences, Oncology and Carcinogenesis, Vaccine Related, Clinical Research, Orphan Drug, Rare Diseases, Pancreatic Cancer, Cancer, Clinical Trials and Supportive Activities, Digestive Diseases, 6.1 Pharmaceuticals, Evaluation of treatments and therapeutic interventions, Albumins, Antineoplastic Combined Chemotherapy Protocols, Benzamides, Carcinoma, Pancreatic Ductal, Deoxycytidine, Female, Follow-Up Studies, Humans, Janus Kinase 1, Janus Kinase 2, Male, Maximum Tolerated Dose, Middle Aged, Paclitaxel, Pancreatic Neoplasms, Prognosis, Pyrimidines, Tissue Distribution, Gemcitabine, JAK inhibitor, Momelotinib, Phase 1, TBK1 inhibitor, Pharmacology and Pharmaceutical Sciences, Oncology & Carcinogenesis, Oncology and carcinogenesis, Pharmacology and pharmaceutical sciences

Abstract

Purpose Preclinical evidence suggests the importance of Janus activating kinase (JAK) and TANK-binding kinase 1 (TBK1) in pancreatic ductal adenocarcinoma (PDAC). We evaluated the safety and efficacy of momelotinib (MMB), a JAK1/2 inhibitor with additional activity against TBK1, plus albumin-bound paclitaxel + gemcitabine (nab-P + G), in patients with previously untreated metastatic PDAC. Experimental Design Patients were enrolled into five cohorts of increasing doses of MMB between 100 and 200 mg administered once or twice daily in combination with nab-P + G in 28-day cycles to determine maximum tolerated dose (MTD). Safety, efficacy, pharmacokinetics, and pharmacodynamics were assessed for all patients. Results Twenty-five patients were enrolled. Dose-limiting toxicities of Grade 3 diarrhea occurred in 1 patient each in the 100 and 200 mg MMB once-daily dose groups. MTD was not reached. The 200 mg MMB twice-daily was the maximum administered dose. Objective response rate was 28% (all partial responses), and 13 (52%) patients had a best response of stable disease. The most common adverse events (AEs) were fatigue (80%), nausea (76%), and anemia (68%). Grade 3 or 4 AEs, most commonly neutropenia (32%), were reported by 88% of patients, of which 44% were considered related to MMB. Pharmacokinetic analyses showed MMB concentrations were too low for TBK1 inhibition. Conclusions MMB was safe and well tolerated in combination with nab-P + G. As no OS or PFS benefit vs nab-P + G was apparent in context of suboptimal engagement of the target TBK1, this study does not support further development of MMB as a first-line therapy in pancreatic cancer.

Published

2019

247. Development of self-assembled multi-arm polyrotaxanes nanocarriers for systemic plasmid delivery in vivo

Author

Ji, Ying, Liu, Xiangsheng, Huang, Max, Jiang, Jinhong, Liao, Yu-Pei, Liu, Qi, Chang, Chong Hyun, Liao, Han, Lu, Jianqin, Wang, Xiang, Spencer, Melissa J, and Meng, Huan

Subjects

Medical Biotechnology, Biomedical and Clinical Sciences, Nanotechnology, Cancer, Genetics, Gene Therapy, Biotechnology, Bioengineering, Adaptive Immunity, Animals, Antineoplastic Agents, Cell Line, Tumor, Cyclodextrins, Drug Carriers, Female, Gene Transfer Techniques, Interleukin-12, Mice, Inbred C57BL, Nanoparticles, Plasmids, Poloxamer, Rotaxanes, Tissue Distribution, alpha-Cyclodextrins, Systemic gene delivery, Multi-arm polyrotaxane, Nanocarrier, Immunoengineering, Immunogenetherapy, Colon cancer, Tumor microenvironment

Abstract

Polyrotaxane (PRX) is a promising supramolecular carrier for gene delivery. Classic PRX exhibits a linear structure in which the amine-functionalized α-cyclodextrin (CD) is threaded along the entire polyethylene glycol (PEG) backbone. While promising in vitro, the absence of free PEG moieties after CD threading compromised the in vivo implementation, due to the unfavorable pharmacokinetics (PK) and biodistribution profile. Herein, we developed a multi-arm PRX nanocarrier platform, which has been designed for protective nucleic acid encapsulation, augmented biodistribution and PK, and suitable for intravenous (IV) administration. A key design was to introduce cationic CD rings onto a multi-arm PEG backbone in a spatially selective fashion. The optimal structural design was obtained through iterative rounds of experimentation to determine the appropriate type and density of cationic charge on CD ring, the degree of PEGylation, the size and structure of polymer backbone, etc. This allowed us to effectively deliver large size reporter and therapeutic plasmids in cancer mouse models. Post IV injection, we demonstrated that our multi-arm polymer design significantly enhanced circulatory half-life and PK profile compared to the linear PRX. We continued to use the multi-arm PRX to formulate a therapeutic plasmid encoding an immunomodulatory cytokine, IL-12. When tested in a colon cancer syngeneic mouse model with same background, the IL-12 plasmid was protected by the multi-arm PRX and delivered through the tail vein to the tumor site, leading to a significant tumor inhibition effect. Moreover, our delivery system was devoid of major systemic toxicity.

Published

2019

248. 18F-labeled anti-human CD20 cys-diabody for same-day immunoPET in a model of aggressive B cell lymphoma in human CD20 transgenic mice

Author

Zettlitz, Kirstin A, Tavaré, Richard, Tsai, Wen-Ting K, Yamada, Reiko E, Ha, Noel S, Collins, Jeffrey, van Dam, R Michael, Timmerman, John M, and Wu, Anna M

Subjects

Biomedical and Clinical Sciences, Clinical Sciences, Oncology and Carcinogenesis, Rare Diseases, Lymphoma, Bioengineering, Biomedical Imaging, Cancer, Hematology, Orphan Drug, 4.1 Discovery and preclinical testing of markers and technologies, Detection, screening and diagnosis, Animals, Antibodies, Antigens, CD20, Fluorine Radioisotopes, Humans, Isotope Labeling, Lymphoma, B-Cell, Mice, Mice, Transgenic, Positron-Emission Tomography, Radiochemistry, Time Factors, Tissue Distribution, Anti-CD20 cys-diabody, Antibody fragments, ImmunoPET, F-18, B cell lymphoma, Same-day imaging, 18F, Other Physical Sciences, Nuclear Medicine & Medical Imaging, Clinical sciences

Abstract

PurposeMetabolic imaging using [18F]FDG is the current standard for clinical PET; however, some malignancies (e.g., indolent lymphomas) show low avidity for FDG. The majority of B cell lymphomas express CD20, making it a valuable target both for antibody-based therapy and imaging. We previously developed PET tracers based on the humanised anti-CD20 antibody obinutuzumab (GA101). Preclinical studies showed that the smallest bivalent fragment, the cys-diabody (GAcDb, 54.5 kDa) with a peak uptake at 1-2 h post-injection and a biological half-life of 2-5 h, is compatible with short-lived positron emitters such as fluorine-18 (18F, t1/2 110 min), enabling same-day imaging.MethodsGAcDb was radiolabeled using amine-reactive N-succinimidyl 4-[18F]-fluorobenzoate ([18F]SFB), or thiol-reactive N-[2-(4-[18F]-fluorobenzamido)ethyl]maleimide ([18F]FBEM) for site-specific conjugation to C-terminal cysteine residues. Both tracers were used for immunoPET imaging of the B cell compartment in human CD20 transgenic mice (hCD20TM). [18F]FB-GAcDb immunoPET was further evaluated in a disseminated lymphoma (A20-hCD20) syngeneic for hCD20TM and compared to [18F]FDG PET. Tracer uptake was confirmed by ex vivo biodistribution.ResultsThe GAcDb was successfully 18F-radiolabeled using two different conjugation methods resulting in similar specific activities and without impairing immunoreactivity. Both tracers ([18F]FB-GAcDb and [18F]FBEM-GAcDb) specifically target human CD20-expressing B cells in transgenic mice. Fast blood clearance results in high contrast PET images as early as 1 h post injection enabling same-day imaging. [18F]FB-GAcDb immunoPET detects disseminated lymphoma disease in the context of normal tissue expression of hCD20, with comparable sensitivity as [18F]FDG PET but with added specificity for the therapeutic target.Conclusions[18F]FB-GAcDb and [18F]FBEM-GAcDb could monitor normal B cells and B cell malignancies non-invasively and quantitatively in vivo. In contrast to [18F]FDG PET, immunoPET provides not only information about the extent of disease but also about presence and localisation of the therapeutic target.

Published

2019

249. Harnessing Androgen Receptor Pathway Activation for Targeted Alpha Particle Radioimmunotherapy of Breast Cancer

Author

Thorek, Daniel LJ, Ku, Anson T, Mitsiades, Nicholas, Veach, Darren, Watson, Philip A, Metha, Dipti, Strand, Sven-Erik, Sharma, Sai Kiran, Lewis, Jason S, Abou, Diane S, Lilja, Hans G, Larson, Steven M, McDevitt, Michael R, and Ulmert, David

Subjects

Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Cancer, Biotechnology, Breast Cancer, Estrogen, 2.1 Biological and endogenous factors, Aetiology, Alpha Particles, Animals, Biomarkers, Tumor, Breast Neoplasms, Cell Line, Tumor, Disease Models, Animal, Dose-Response Relationship, Drug, Dose-Response Relationship, Radiation, Female, Hexokinase, Humans, Immunoconjugates, Mice, Molecular Targeted Therapy, Radioimmunotherapy, Radiometry, Receptors, Androgen, Signal Transduction, Tissue Distribution, Xenograft Model Antitumor Assays, Oncology & Carcinogenesis, Clinical sciences, Oncology and carcinogenesis

Abstract

PurposeThe impact of androgen receptor (AR) activity in breast cancer biology is unclear. We characterized and tested a novel therapy to an AR-governed target in breast cancer.Experimental Design: We evaluated the expression of prototypical AR gene products human kallikrein 2 (hK2) and PSA in breast cancer models. We screened 13 well-characterized breast cancer cell lines for hK2 and PSA production upon in vitro hormone stimulation by testosterone [dihydrotestosterone (DHT)]. AR-positive lines were further evaluated by exposure to estrogen (17β-Estradiol) and the synthetic progestin D-Norgestrel. We then evaluated an anti-hK2-targeted radiotherapy platform (hu11B6), labeled with alpha (α)-particle emitting Actinium-225, to specifically treat AR-expressing breast cancer xenografts under hormone stimulation.ResultsD-Norgestrel and DHT activated the AR pathway, while 17β-Estradiol did not. Competitive binding for AR protein showed similar affinity between DHT and D-Norgestrel, indicating direct AR-ligand interaction. In vivo production of hK2 was sufficient to achieve site-specific delivery of therapeutic radionuclide to tumor tissue at >20-fold over background muscle uptake; effecting long-term local tumor control.Conclusions[225Ac]hu11B6 targeted radiotherapy was potentiated by DHT and by D-Norgestrel in murine xenograft models of breast cancer. AR activity in breast cancer correlates with kallikrein-related peptidase-2 and can be activated by D-Norgestrel, a common contraceptive, and AR induction can be harnessed for hK2-targeted breast cancer α-emitter radiotherapy.

Published

2019

250. APOE Effect on Amyloid-β PET Spatial Distribution, Deposition Rate, and Cut-Points.

Author

Toledo, Jon B, Habes, Mohamad, Sotiras, Aristeidis, Bjerke, Maria, Fan, Yong, Weiner, Michael W, Shaw, Leslie M, Davatzikos, Christos, and Trojanowski, John Q

Subjects

Biomedical and Clinical Sciences, Biological Psychology, Clinical Sciences, Neurosciences, Psychology, Aging, Brain Disorders, Acquired Cognitive Impairment, Clinical Research, Dementia, Alzheimer's Disease including Alzheimer's Disease Related Dementias (AD/ADRD), Alzheimer's Disease, Neurodegenerative, Biomedical Imaging, Aetiology, 2.1 Biological and endogenous factors, Detection, screening and diagnosis, 4.1 Discovery and preclinical testing of markers and technologies, Neurological, Aged, Aged, 80 and over, Alzheimer Disease, Amyloid beta-Peptides, Apolipoprotein E4, Apolipoproteins E, Biomarkers, Cognitive Dysfunction, Cross-Sectional Studies, Female, Genotype, Humans, Longitudinal Studies, Male, Middle Aged, Positron-Emission Tomography, Reference Values, Sex Characteristics, Tissue Distribution, Alzheimer's disease, amyloid-beta, cerebrospinal fluid, diagnosis, mild cognitive impairment, positron emission tomography, Alzheimer’s Disease Neuroimaging Initiative, Alzheimer’s disease, amyloid-β, Cognitive Sciences, Neurology & Neurosurgery, Clinical sciences, Biological psychology

Abstract

There are conflicting results regarding how APOE genotype, the strongest genetic risk factor for Alzheimer's disease (AD), influences spatial and longitudinal amyloid-β (Aβ) deposition and its impact on the selection of biomarker cut-points. In our study, we sought to determine the impact of APOE genotype on cross-sectional and longitudinal florbetapir positron emission tomography (PET) amyloid measures and its impact in classification of patients and interpretation of clinical cohort results. We included 1,019 and 1,072 Alzheimer's Disease Neuroimaging Initiative participants with cerebrospinal fluid Aβ1 - 42 and florbetapir PET values, respectively. 623 of these subjects had a second florbetapir PET scans two years after the baseline visit. We evaluated the effect of APOE genotype on Aβ distribution pattern, pathological biomarker cut-points, cross-sectional clinical associations with Aβ load, and longitudinal Aβ deposition rate measured using florbetapir PET scans. 1) APOEɛ4 genotype influences brain amyloid deposition pattern; 2) APOEɛ4 genotype does not modify Aβ biomarker cut-points estimated using unsupervised mixture modeling methods if white matter and brainstem references are used (but not when cerebellum is used as a reference); 3) findings of large differences in Aβ biomarker value differences based on APOE genotype are due to increased probability of having AD neuropathology and are most significant in mild cognitive impairment subjects; and 4) APOE genotype and age (but not gender) were associated with increased Aβ deposition rate. APOEɛ4 carrier status affects rate and location of brain Aβ deposition but does not affect choice of biomarker cut-points if adequate references are selected for florbetapir PET processing.

Published

2019